Authors: Ana Margarida Gonçalves, Patricia Monteiro
Categories: Neurology and Preclinical Neurological Studies - Review Article, Auditory, Autism spectrum disorder (ASD), Neuroscience, Patients, Sensory
Source: Journal of Neural Transmission
Authors: Ana Margarida Gonçalves, Patricia Monteiro
Autism Spectrum Disorder (ASD) is a neurodevelopmental condition with a wide spectrum of symptoms, mainly characterized by social, communication, and cognitive impairments. Latest diagnostic criteria according to DSM-5 (Diagnostic and Statistical Manual of Mental Disorders, Fifth Edition, 2013) now include sensory issues among the four restricted/repetitive behavior features defined as “hyper- or hypo-reactivity to sensory input or unusual interest in sensory aspects of environment”. Here, we review auditory sensory alterations in patients with ASD. Considering the updated diagnostic criteria for ASD, we examined research evidence (2015–2022) of the integrity of the cognitive function in auditory-related tasks, the integrity of the peripheral auditory system, and the integrity of the central nervous system in patients diagnosed with ASD. Taking into account the different approaches and experimental study designs, we reappraise the knowledge on auditory sensory alterations and reflect on how these might be linked with behavior symptomatology in ASD.
Autism spectrum disorder (ASD) is a neurodevelopment condition characterized by deficits in social communication and interaction, and restricted/repetitive behavioral features (Peça et al. 2011), showing first symptoms typically around three years old (Robertson and Baron-Cohen 2017). In 2018, the Centers for Disease Control and Prevention (CDC) reported approximately one in 44 children diagnosed with ASD, with a four times higher prevalence in boys versus girls. There is a wide variation in the type and severity of symptoms in ASD. Unlike other diagnoses, such as a specific phobia, it is not easy to draw a straight line from symptoms to diagnostic criteria. Each neurodivergent individual with ASD is unique, and the diagnosis is based on behavioral observation.
The year 2013 was an important landmark for Autism conceptualization, with the release of the latest version of the Diagnostic and Statistical Manual of Mental Disorders (DSM–5) (American Psychiatric Association (APA) 2013). Before DSM-5, there were poor diagnostic criteria with limited reliability in assigning subcategory diagnosis (Walker et al. 2004). The diagnosis of autism was categorized by subcategories (e.g., autistic disorder, Asperger’s disorder, and pervasive developmental disorder not otherwise specified). With the fifth edition of DSM, there was an important shift in the conceptualization of Autism became a single diagnosis based on multiple dimensions. The DSM-5 refers to Autism as a Spectrum Disorder, embracing an umbrella of symptoms with wide variety and severity levels. The new diagnosis of ASD includes persistent deficits in social communication and social interaction across multiple contexts, and restricted and repetitive patterns of behavior, interests, or activities (American Psychiatric Association (APA) 2013). These symptoms are present in early developmental period, significantly interfering with individuals’ daily functioning (American Psychiatric Association (APA) 2013).
In 2018, the World Health Organization updated the classification of autism in the International Classification of Diseases (ICD-11) (Organization 2018), to be more in line with DSM-5. The latest version of ICD-11 came into effect on January 2022 (Organization 2018). Both authoritative guidebooks used by medical professionals for the diagnosis and treatment of diseases and disorders collapse autism into a single diagnosis of Autism Spectrum Disorder, embracing the same two major difficulties in initiating and sustaining social communication and social interaction, and restricted interests and repetitive behaviors (Rosen et al. 2021).
The evolution of Autism criteria diagnosis reflects the evolving concern of clinicians and, particularly, researchers. If the diagnostic criteria are not easily well defined, people with autistic-like traits might be included, leading to misleading clinical cohorts that might hinder a clear understanding of autism neurobiology. As an example, as DSM-IV (American Psychiatric Association (APA) 1994), the previous version of the International Classification of Diseases, ICD-10 (Organization 1993), included a third category for language problems. The ICD-10 subdivided communication and social interaction into different clusters. Given that clinicians found it hard to categorize symptoms as either, both DSM-5 and ICD-11 now combine social and language deficits into a single measure. These deficits seem to be interrelated, being understood that a child with limited language or communication problems would have limited social interaction. However, the cause of these communication and language impairments is still unclear.
Over the years, the focus of ASD diagnosis was mainly related to cognitive, communication, and social impairments. But more recently, the criteria of diagnosis started to include another the sensory processing domain (Robertson and Baron-Cohen 2017). The DSM-5, and more recently the ICD-11, now include sensory hyper- and hypo-sensitivities as part of the restricted and repetitive behavior domain (American Psychiatric Association (APA) 2013; Organization 2018). Atypical responses to sensory stimuli can also help to differentiate ASD from other developmental disorders (Stewart et al. 2016).
Sensory integration is a neurobiological process that refers to the integration and interpretation of sensory stimuli from surrounding context to the brain. Atypical sensory experience seems to occur in 85% of individuals with ASD and can be noticeable early in development (Robertson and Baron-Cohen 2017). Symptoms can include hypersensitivity, avoidance, diminished responses, or even sensory seeking behavior (Robertson and Baron-Cohen 2017; Sinclair et al. 2017). These alterations in sensory processing may interfere with the typical development of higher order functions such as social communication, which requires quick, accurate integration of sensory cues in real time (Robertson and Baron-Cohen 2017; Siemann et al. 2020). Many studies have looked into multisensory processing, highlighting the role of temporal binding windows as a critical factor in information integration (Robertson and Baron-Cohen 2017). The concept of temporal binding window refers to a window of time where specific modalities are perceptually bound (Hillock et al. 2011). A recent review from Siemann and colleagues describes numerous findings related to the presence of multisensory and temporal processing deficits in individuals with ASD (2020) (Siemann et al. 2020), suggesting atypical multisensory temporal processing with increased stimulus complexity. Although atypical sensory processing can be present across several sensory domains, atypical behavioral response to environmental sounds is among the most prevalent and disabling sensory feature of autism, with more than 50% of individuals exhibiting impaired sound tolerance (Williams et al. 2021).
Many individuals diagnosed with ASD have auditory sensitivities, and it is common to observe children with ASD covering their ears, even in the absence of salient background noise. Individuals with ASD can present hyper- or hypo-sensitivity to a variety of sensory stimuli, which can cause a wide range of behavioral manifestations and maladaptations (Sinclair et al. 2017). Children underresponsive to sensory input appear to be unaware of auditory stimuli that are salient to others. Studies have shown that pronounced to profound bilateral hearing loss or deafness seems to be present in 3.5% of all cases, and hyperacusis (increased sensitivity or decreased tolerance to sound) affects nearly 18–40% of children with autism (Williams et al. 2021; Rosenhall et al. 1999; Wilson et al. 2017). Individuals with auditory hypersensitivity can notice auditory stimuli at intensity levels that are not salient or would not trouble others, which may cause sensory overload. For a person experiencing sensory overload, everyday sounds can be unpleasant and overwhelming, and that may lead to poor emotional and social regulation (Wilson et al. 2017), with impairments at the level of filtering out irrelevant input. The appropriate filtering of sensory information is crucial for healthy brain function, allowing salient awareness and focus on relevant social cues. Deficits in auditory processing can thus affect behavior, with profound effects on a person’s life, especially in the development of higher level skills such as social communication. However, the knowledge about phenomenology or neurocognitive underpinnings that underlie these auditory sensory processing deficits is still scarce. In fact, many studies have been performed before DSM-5 criteria, having a confound effect of potential misdiagnosis or comorbidity with other disorders.
To avoid such potential confounds, we opted for a systematic review of auditory sensory function in patients with ASD, considering studies performed between 2015 and 2022 (2 years after DSM-5 implementation), thus considering the recent adaption of autism diagnosis as a spectrum disorder.
The following questions will be A.What is known about the integrity of Cognitive Function in auditory-related tasks?B.What is known about the integrity of Peripheral Auditory System in auditory-related tasks?C.What is known about the integrity of Central Auditory Nervous System in auditory-related tasks?
This systematic review follows the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines (Page et al. 2021), and review methods were established before initiating literature screening.
The search strategy started in September 2021 and used MeSH terms from PubMed. Used PubMed, Web of Science (all databases/collections), Scopus, and Scielo. Search terms included “autis*” AND “auditory”, and were limited to studies published between 2015 and March of 2022. The minimum year of 2015 was considered as the mark of first experimental studies using DSM-5 as a diagnosis of Autism Spectrum Disorders (American Psychiatric Association (APA) 2013).
Studies were eligible if they consisted of original and reported data, with comparison group design, written in English and published in peer-reviewed journals. Conference abstracts, books and documents, editorials, letters, pilot studies, case studies, reviews, and meta-analyses were excluded.
Only studies with human participants with a clear diagnosis of ASD were considered. To avoid confounding results, studies with ASD participants that were also diagnosed with other symptomatology and/or disorders were epilepsy, Williams Syndrome, ADHD, Rett Syndrome, Angelman Syndrome, Fragile X Syndrome, etc. Participants diagnosed with ASD in early childhood but without current ASD symptoms, or participants with the diagnosis based on the DSM-IV without other assessments of diagnosis validation (e.g., ICD-11 and ADOS) were also excluded. No restrictions of age, gender, racial, ethnic, and socioeconomic groups were made.
Studies that did not include relevant outcome data were excluded (e.g., ASD parents’ symptomatology; studies focused on visual processing that used auditory cues in the task that are not referred to in the results; studies focused on pilot training or intervention programs).
Most of the tools used to confirm ASD diagnosis in the studies included on this review Short-Sensory Profile (SPP) (Dunn 1999), Childhood Autism Rating Scale (CARS) (Schopler et al. 2010), Autism Diagnostic Observation Schedule, Second Edition (ADOS-2) (Lord et al. 2012), and the Peabody test (Dunn and Dunn 1965). To estimate global intellectual ability (full-scale IQ), most tests used were the Wechsler Adult Intelligence Scale or the Wechsler Intelligence Scale for Children (Wechsler and Kodama 1949), and Raven’s Colored Progressive Matrices Test (Measso et al. 1993). Even if there is no official diagnosis for ASD being described as low or high functioning, some papers identified some ASD groups as being high-functioning autism (usually subjects with an IQ mean higher than 85).
Cognitive function can be assessed by mental processes such as perception, attention, memory, decision-making, or language comprehension, and in the domain of social cognition (e.g., theory of mind, social and emotional processing). People with ASD have a profile of cognitive strengths and weaknesses, demonstrated by different levels of deficits in social and non-social cognition patterns. To understand how auditory input might influence cognitive function in ASD, it is useful to assess cognitive integrity at several domains, while performing auditory-related tasks.
Communication in everyday life depends crucially on the ability to detect stimuli and dynamically shift attention between competing auditory streams. We use attention to direct our perceptual systems toward certain stimuli for further processing. Difficulties in attention processes can directly affect social interaction and communication abilities. When compared to neurotypical controls, individuals with ASD seem to have poorer performance in many auditory attention divided attention (ability to attend to two or more stimuli at the same time), sustained attention (ability to attend stimulus over longer periods), selective attention (ability to ignore details of stimulus not attended), and spatial attention (selecting a stimulus based on its spatial location). Main findings are summarized in Table 1.Table 1Summary results of attention studies, organized by type of attentionType of attentionStudyIQ assessmentMean age (SD)ExperimentTestCognitive standard scoresMean (SD)ASDTaskResults ASDDIVIDEDFoster et al. (2016)WASIIQ > 7012.9 y (2.5)Direct and Divided attentionLess sensitive to global interferenceSUSTAINEDCrasta et al. (2020)WASI112 (12.37)8.24 (1.39)TEA-ChTEA-Ch: worst scores in Sustained and Control attentionSustained and control attentionPastor-Cerezuela et al. (2020)Raven, PeabodyNon-verbal: 100.88 (lv 2)81.20 m (11.18)Nepsy-IISustained-attention: worst performanceVerbal: 72.68 (18.19)Maintain vs sustained attentionSELECTIVEEmmons et al. (2022)WASI-II102.36 (14.33)21.75 y (0.64)Selective vs maintain-listeningNo differences between hold and maintain tasks worst accuracy at both compared with TDSPATIALSoskey et al. (2017)WISC-IV111 (12.30)13.78 y (1.93)Target and distractor soundsDiffuse auditory spatial attention across all stimulus types more front target | increased responding to sounds at adjacent non-target locationsDIVIDED attention ability to attend two or more stimuli at the same time, SUSTAINED attention ability to attend stimulus over long periods, SELECTIVE attention ability to ignore details of stimulus not attended, SPATIAL attention involves selecting a stimulus on the basis of its spatial locationRaven Raven Colored Progressive Matrices Test, *Peabody *Peabody picture vocabulary test, *TEA-Ch *Test of Everyday Attention for Children, lv 2 level 2 of severity, vs versus, y years, m months
Low-level auditory discrimination ability seems to vary widely within ASD. When different paradigms were compared, no differences were found for adults with ASD regarding selective attention (maintain vs switch tasks) (Emmons et al. 2022). However, infants and children with ASD presented poorer performances for sustained and control attention, attentional disengagement, and reorienting (Keehn et al. 2021), when compared with typically developing peers (TD). Spatial attention, a key component for social sound orientation, was measured by looking at central or peripheral locations of target sounds location while ignoring nearby sounds (Soskey et al. 2017). Adults diagnosed with ASD show diffuse auditory spatial attention independently of stimulus simple tones, speech sounds (vowels), and complex non-speech sounds (Soskey et al. 2017). Interestingly, children with ASD show more diffuse auditory spatial attention, indicated by increased responding to sound at adjacent non-target locations (Soskey et al. 2017). Subjects with ASD also seem to be less sensitive to global interference, or mixed cues, when compared with just one cue (local targets processed slower due to the presence of inconsistent global information) (Foster et al. 2016).
Information from different sensory modalities, such as auditory and visual stimuli, can be easily integrated simultaneously by the nervous system. The visual sensory system of ASD individuals seems to be similar to TD peers, as opposed to their auditory system (Little et al. 2018). Different sensory modalities combined can create multisensory facilitation. As an example, speech perception is boosted when a listener can see the mouth of a speaker and integrate auditory and visual speech information. However, multisensory integration (MSI) is thought to be distinctive in ASD (Ainsworth et al. 2020) (Table 2), with temporal processing deficits that are not generalized across multiple sensory domains (Ganesan et al. 2016).Table 2Summary results of multisensory integration, organized by level of perceptual processPerceptual processExperimentIQ assessmentMean age (SD)StudyParadigmStimuliResultsTestCognitive standard scoresMean (SD)ASDLLPoole et al. (2021)Determine whether the stimulus was continuous or pulsed on each trialVisual, tactile and auditoryASD: shift costs were observed for each target modality in participant response times—> conditions called target – previous targetASD: largest for auditory targets (auditory repeat trials) when compared with visual and tactile targetsWeschler118.41 (10.15)30.58 (7.40)LLAinsworth et al. (2021)Target detection taskAuditory (A; 3500 Hz tone), visual (V; white disk ‘flash’) or audiovisual (mix of both)ASD showed reduced multisensory facilitation compared to NT participants in a simple target detection task, void of social contextWISC-IV112.85 (17.89)11.91 (2.00)WASI-II107.16 (11.57)19.05 (4.10)LLOstrolenk et al. (2019)RTs on the audiovisual conditionVisual and auditory non-social stimuli (i.e., flashes and beeps)MSI of simple information, void of social content or complexity, altered in autismWeschler102.95 (13.71)19.21 (4.71)LLStewart et al. (2016)Determine whether the stimulus was high (tone/visual position) or lowUnisensory auditory, unisensory visual, and bisensory (congruent auditory and visual stimuliReduced response times for bisensory compared to unisensory trials were seen in both ASD and control groupsWASI109.4 (15.3)12.8 (2.9)LL + HLRighi et al. (2018)Eye tracking (sensitivity to temporal asynchronies in a speech processing)Videos synchronized (or not) with audioASD: failed to demonstrate sensitivity to asynchronies of 0.3 s, 0.6 s, or 1.0 sBayley69.73 (25.43)5.12 (1.53)Correlated with language abilities—measured by PLSWPPSIStanford BinetLL + HLNoel et al. (2017)Simultaneity judgment (asynchronous audiovisual stimuli of varying levels of complexity)Simple and non-linguistic stimuli (i.e., flashes and beeps, hand-held tools) and speech stimuliASD fail to rapidly recalibrate to audiovisual asynchronies simple and non-linguistic stimuli, but exhibit comparable rapid recalibration for speech stimuliWASI-2110.23 (14.05)HLFoss-Feig et al. (2017)Psychophysical gap detection taskVisual and auditoryDomain-specific impairment in rapid auditory temporal processing in ASD that is associated with greater difficulties in language processingWeschler115.96 (17.4)11.94 (1.3)Auditory taskHLSmith et al. (2017)Temporal window of IntegrationBasic speech (consonant–vowel utterances) and object stimuli (bouncing ball)ASD: less tolerance of asynchrony for speech stimuli compared to object stimuliWeschler111.45 (15.57)14.55 (2.18)HLChahboun et al. (2016)Cross-modal sentence- picture matching taskFigurative expressions and their target figurative meaning represented in imagesASD displayed higher error rates and greater reaction latencies in the auditory modality compared to the visual stimulus presentation modalityWISC-IV110.71 (14.58)11.3 (0.96)WAIS-IV108.3 (13.39)18.1 (1.65)HLTuri et al. (2016)Instantaneous adaptation to audiovisual asynchronyVisual and auditory stimuli, varying in asynchrony over a wide range, from 512 ms auditory-lead to 512 ms auditory-lagTypical adults showed strong adaptation effectsWeschler112.0 (10.32)29.2 (5.2)LL Low Level Perceptual Process, HL High Level Perceptual Process, Bayley Bayley Scales of Infant Development, Stanford Binet Stanford Binet Intelligence Scales, Weschler Weschler Full-Scale IQ, WPPSI Wechsler Preschool and Primary Scale of Intelligence-III, PLS Preschool Language Scales
An experimental design based on Miller’s race model (Miller 1982) was tested by assessing the accuracy and reaction times of unisensory and bisensory (visual and auditory) trials and by comparing children with ASD with typically developing peers (TD) as a control group (Stewart et al. 2016). Findings did not support impaired bisensory processing for simple non-verbal stimuli in high-functioning children with ASD (Stewart et al. 2016). Reduced bisensory facilitation was found for both ASD and TD groups, suggesting intact low-level audiovisual integration. Another study assessed the reaction time of target stimuli detection task (auditory, 3500 Hz tone; visual, white disk ‘flash’; and audiovisual, simultaneous tone and flash) by comparing younger (age 14 or younger) and older participants (age 15 and older) (Ainsworth et al. 2020). The authors found greater multisensory reaction time facilitation for neurotypical (NT) adults, increased for older participants, and reduced multisensory facilitation for ASD, both in younger and older participants.
Audiovisual integration of basic speech and object stimuli was compared in children and adolescents diagnosed with ASD (Smith et al. 2017). To measure audiovisual perception, a temporal window of integration was established, where individuals identify which video (temporally aligned or not) matched the auditory stimuli. Results showed similar tolerance of asynchrony for the simple speech and object stimuli for controls, while ASD adolescents showed decreased tolerance of asynchrony for speech stimuli. These results were associated with higher levels of symptom severity (Smith et al. 2017). A similar result of instantaneous adaptation to audiovisual asynchrony was found in ASD adults (Turi et al. 2016). This means that reduced adaptation effect in ASD individuals, and poorer multisensory temporal acuity, may be hindering speech comprehension and consequently affecting social communication.
Social interaction implies attentional shift, such as joint attention (when a person intentionally focuses attention on another person). A study tested whether impairments in joint attention were influenced by self-relevant processing. Results showed that gaze-triggered attention is influenced by self-relevant processing and symptom severity in ASD individuals, with reduced cueing effect to voice compared to tone targets (Zhao et al. 2019).
The stimulus presentation modality can lead to differences in figurative language comprehension, even with high-verbal ASD individuals (matched with TD peers on intelligence and language level) (Chahboun et al. 2016). When visual and auditory modalities are compared, individuals with ASD present the poorest performances in the auditory modality, showing difficulties to understand culturally based expressions (Chahboun et al. 2016). Greater difficulties in language processing seem to be correlated with higher auditory gap detection thresholds (minimum interval between sequential stimuli needed for individuals to perceive an interruption between the stimuli) (Foss-Feig et al. 2017).
Multisensory facilitation can be highly valuable, especially in noisy environments. A diminished capacity to integrate sensory information across modalities can potentially contribute to impaired social communication.
Cognitive performance in ASD was assessed with experimental manipulation of noise (quiet and 75 dB gated broadband noise) adding different levels of task difficulty (easier and harder) (Keith et al. 2019). Results show that for NT adolescents, it is easier to adapt to the effect of noise. In contrast, the ASD group shows a detrimental effect of noise and increased arousal in the harder condition (Keith et al. 2019). Children with ASD who attend more time to the stimulus, such as looking longer to the speaker’s face, show better listening performance (Newman et al. 2021). When different levels of signal-to-noise ratio (SNR) are compared, ASD and NT groups exhibited greater benefit at low SNRs relative to high SNRs in phoneme recognition tasks (Stevenson et al. 2017). The ASD group shows a reduced performance in both auditory and audiovisual modalities for whole-word recognition tasks with high SNRs (Stevenson et al. 2017), when compared with TD peers. High-functioning ASD adults show a speech comprehension rate of nearly 100% in the absence of noise, similar to IQ-matched controls (Piatti et al. 2021; Dwyer et al. 2021). However, under noise conditions, the ASD group presents worse speech comprehension and neural over-responsiveness (Piatti et al. 2021; Dwyer et al. 2021). Such results suggest that noise may increase the threshold needed to extract meaningful information from sensory inputs, affecting speech comprehension.
Regarding auditory perceptual capacity, there is a wide variety of experimental designs, paradigms, and tested parameters, holding different results (Table 3). When ASD and TD individuals were compared, significant differences were found in the ASD group regarding several acoustic parameters, such as deficits in the intensity or loudness of stimuli, higher auditory duration discrimination threshold of stimuli, and enhanced memory for vocal melodies (Kargas and Lo 2015; Isaksson et al. 2018; Weiss et al. 2021). Musical and vocal timbre perception seems to be intact for older ASD participants (Schelinski et al. 2016), with one study showing decreased music ability, related with deficits at the level of working memory and hyperactivity/inattention of young ASD children (Sota et al. 2018).Table 3Summary results of auditory detection and discrimination studies, organized by yearExperimentIQ assessmentMean age (SD)StudyParadigmStimuliResultsTestCognitive standard scoresMean (SD)Or Mean age (range)ASDWeiss et al. (2021)Memory for vocal and instrumental melodiesVocal (e.g.. la, la) and instrumental (piano, marimba) melodiesASD: Enhanced Memory for Vocal MelodiesWASI104.4 (19.2)11.1 (1.4)Schelinski et al. (2019)Vocal Emotion Recognition Test, Vocal Pitch and Vocal Timbre Discrimination Test, Non‐vocal Pitch Perception TestAuditorily presented words (65 dB)Vocal impaired ASDWAIS-III110.31 (13.79)33.75 (10.12)ND for ASD: pitch, timbreGermain et al. (2018)Low-level pitch directionPairs of tones that differed in pitch and were presented at various temporal rates (pure sine tones + harmonics)Pitch direction perception predicts global–local pitch processing (individual differences in low-level pitch direction ability predicted performance on the higher level global–local task, with a stronger relationship in ASD)WASI110.813.7 (2.3)High-level global–local taskThree-tone triplet sequences combined to form sequences of nine harmonic tonesIsaksson et al. (2018)Motor and perceptual timingFree tapping, simultaneity judgment, auditory duration discrimination, and verbal duration estimationAuditory duration discrimination higher for ASDWISC-V102 (18)11:0 (2:4)Dinosaur computer taskASD with abnormalities in temporal processing motor timing, perceptual timing, and temporal perspectiveYears:monthsSota et al. (2018)Musical abilityMBEAASD: Musical ability decreasedWeschler88.85 (12.24)8.62 (2.47)Working memory and hyperactivity/inattention predicted musical abilityChowdhury et al. (2017)Relationship between auditory pitch perception and verbal and non-verbal cognitive abilities in ASD versus TD childrenPairs of tones that differed in pitch and were prompted to choose whether the second tone had a lower or higher pitchNo group differences in performanceWeschler110.8 (18.3)Significant variability in performance on the auditory tasksAuditory perception is related to non-verbal reasoning rather than verbal abilitiesPark et al. (2017)Visual orientation discrimination in the presence of varying levels of external noiseCoarse orientation discrimination task sandwiched by noise stimuliASD: increased internal noise and worse external noise filteringWeschler110.1413.49 (2.08)Measuring perceptual sensitivity across varying levels of external noiseInternal noise significantly correlating with ASD symptoms (ADOS)Remington and Fairnie (2017)Detection and identification tasksExp1. dual-task paradigm (target sounds, dog bark; + non- target, duck)ASD better at detecting additional unexpected and expected soundsWeschler110 (13)30 (3.6)(Highlight both the benefits and disadvantages of increased capacity)Exp2. 69 s auditory sceneIncreased distraction and superior performanceHaigh et al. (2016)Auditory modulation-depth discrimination taskVisual (grating patches) + Auditory (tones)No evidence of atypical sensory function or atypical attentional modulationWeschler114.8 (13.4)27 (21–42)Schelinski et al. (2016)Unfamiliar voice discrimination test, Famous voice recognition test, Acoustic voice feature processing testUVL (voice-face learning; voice-name learning; voice-color learning); ACF (pitch and timbre)ASD: difficulties with discriminating, learning, and recognizing unfamiliar voices (particularly pronounced for learning novel voices)WAIS107.38 (17.55)33.75 (10.12)ASD: deficit in vocal pitch perceptionASD: intact acoustic processing (musical pitch, musical, and vocal timbre perception)Familiar NDMayer et al. (2016)Different pitch discrimination trajectoriesComplex tones and speech pitchPitch discrimination increased with age (TD). ASD: enhanced childhood and stable in adultsRavens34.67 (5–75th percentile)126.07 m (47.53)165.64 (23.46)Monosyllabic words + pitch contours derived from these words482.79 (136.00)Boets et al. (2015)Right versus left auditory cortex processingFrequency discrimination and slow amplitude modulation (AM) detection versus gap-in-noise detection and faster AM detectionASD: impaired frequency discriminationWISC-III-NL > 80(12–19)Target right auditory cortex processing (frequency discrimination, 4 Hz AM) and left auditory cortex processing (gap-in-noise detection, 20 Hz AM)Gap- in-noise detection poorer temporal resolution for ASDNot support the hypothesis of superior right and inferior left hemispheric auditory processing in ASDJiang et al. (2015)Discrimination and identificationMelodic contour and speech intonationASD: superior melodic contour identification but comparable contour discriminationRavens119.12 (13.77)9.41 (3.03)ASD performed worse than controls on both discrimination and identification of speech intonationVIQ116.06 (27.17)Kargas et al. (2015)Loudness, pitch, duration (intensity, frequency and duration)Standard pure tone (74 dB) and a probe tone (55 to 73.5 dB)Significant deficits in ASD on all acoustic parametersWASI109.8 (18.2)30.3 (10.4)Low-level auditory discrimination ability varies widely within ASD—> this variability relates to IQ level, and influences the severity of RRBsRavens Ravens Progressive Matrices, Weschler Weschler Full-Scale IQ, UFV Unfamiliar voice discrimination test, AVF Acoustic voice feature processing test, TD typical development, ND no differences, RRBs restricted and repetitive behaviors, MBEA Montreal Battery of Evaluation of Amusia
One of the common parameters used to test auditory perceptual capacity is pitch detection, the degree of highness, or lowness of a tone. Studies have shown a heightened pitch detection in the ASD group, for expected and unexpected sounds (Remington and Fairnie 2017). Regarding the developmental trajectory of pitch perception, findings reveal enhanced pitch discrimination in childhood with stability across development in ASD (Mayer et al. 2014). Interestingly, this low-level auditory ability seems to vary widely within ASD, being related to IQ level and severity of symptoms (Kargas and Lo 2015). Adults diagnosed with ASD show superior pitch perception associated with sensory deficits (Mayer et al. 2014). Individual differences in low-level pitch discrimination tasks can predict performance on the higher level global–local tasks (Germain et al. 2018). Results seem to vary between detection and discrimination tasks across studies. A discrimination task assesses the ability to detect the presence of a difference between two or more stimuli. Interestingly, no differences were found between low and higher level pitch processing (Chowdhury et al. 2017) when ASD children were matched in terms of IQ levels and verbal and non-verbal cognitive abilities, as measured by WASI subtests yield (Wechsler and Kodama 1949). For ASD adults without intellectual impairment, when participants were asked to identify modulation-depth differences (e.g., − 3 dB), no differences were found in auditory modulation–depth discrimination tasks (Haigh et al. 2016). ASD adults showed difficulties in discriminating, learning, and recognizing unfamiliar voices (particularly pronounced for learning novel voices) (Schelinski et al. 2016). These results may allow us to speculate that an increased auditory capacity, such as heightened pitch detection, may lead to better performance at detection or discrimination tasks, but may also entail a sensory overload, greatly enhancing the difficulty of the task for different stimuli parameters.
Atypical sound perception and auditory processing deficits may underlie language and learning difficulties in ASD, impairing social communication skills. Studies have found that ASD patients tend to display worst performance in whispered speech compared to normal speech (Venker et al. 2019; Georgiou 2020) and several differences have been reported in terms of language processing and speech perception (Table 4).Table 4Summary results of language assessment, organized by yearSourceExperimentCognitive standard scoresMean age ± SDParadigmStimuliResults ASDTestMean (SD)ASDGeorgiou (2020)Identification of native vowel in normal and whispered speechGreek vowels (/i e a o u/) embedded in a monosyllabic / pVs/ contextSlower in the whispered speechRaven > 40 out of 6031.2 y (4.5)Children with weaker receptive language showed a smaller head start than children with stronger receptive language skillsVenker et al. (2019)Incremental language processing and receptive language (longitudinal)Semantically-constraining verbs (e.g., Read the book) compared to neutral verbs (e.g., Find the book)Head start when presented with semantically-constraining verbsMullen77.06 (26.80)56.15 m (3.94)Noel et al. (2018)Simultaneity judgment task to index their audiovisual temporal acuity for speech stimuliSyllable /ba/ or /ga/ (audio and visual components)Wider window of audiovisual temporal integrationTONI-4106.34 (18.34)12.20 y (3.75)Stevenson et al. (2018)Temporal order judgment taskWhite visual rings on a black background paired with auditory pure-tone beepsTemporal processing abilities in children with autism contributed to impairments in speech perceptionWASI-II–12.3 y (3.1)Foss-Feig et al. (2017)Visual and auditory temporal processing abilitiesGap detection tasks to measure gap detection thresholdsHigher auditory gap detection thresholdsWechsler115.96 (17.4)11.94 (1.3)Correlated significantly with several measures of language processingm months, y years
The integration of information for successful language processing and speech comprehension relies on precise and accurate temporal integration of auditory and visual cues. Children with ASD seem to possess a wider window of audiovisual temporal integration (Stevenson et al. 2017; Noel et al. 2017), and higher auditory gap detection thresholds (Foss-Feig et al. 2017). Deficits at the level of temporal integration may contribute to impaired speech perception. Studies of auditory processing and language paradigms show that language processing can be facilitated in children with ASD using contextual references such as semantically-constrained verbs compared to neutral verbs (Venker et al. 2019).
Language components, such as phonemes, syntax, and context, work together with features to create meaningful communication among individuals. All languages use pitch and contour to carry information about emotions and to communicate non-verbally. The way we say something affects its meaning, just by using different emphasis and intonation. Phonological use of pitch dissimilarities is distinct between tone and non-tone languages at several levels of their phonological hierarchy (prosodic word, phonological phrase, intonational phrase, and utterance tiers) (Beckman and Pierrehumbert 1986). Tones are associated with lexical meaning to distinguish words. English, as a non-tone language, uses contrastive pitch specifications at a segmental level, to express syntactic, discourse, grammatical, and attitudinal functions. A tone language, like Mandarin, uses constructive pitch specifications at every level of the phonological hierarchy (Best 2019). Pitch processing was assessed in individuals who speak Mandarin, by testing melodic contour and speech intonation (Jiang et al. 2015). ASD individuals presented superior melodic contour but comparable contour discrimination, and when compared with controls, ASD performed worse on both identification and discrimination of speech intonation (Jiang et al. 2015), suggesting a differential pitch processing in music that does not compensate for speech intonation perception deficits.
Many studies focusing on language processing use electroencephalography (EEG) to measure brain activity in real time. EEG signals reflect electrical activity produced by the brain (brain waves). An approach known as event-related potential (ERP), uses EEG activity that is time-locked with ongoing sensory, motor, or cognitive events, to help identify and classify perceptual, memory, and linguistic operations (Sur and Sinha 2009). To avoid confounding effects in the interpretation of ERP results, most studies only include children with normal or corrected-to-normal vision, normal hearing, and absence of genetic or neurological disorders, history of seizures, or past head injury. To check for hearing disabilities, many studies also perform a hearing screening with pure-tone audiometry at 20 dB. However, there is a wide variation regarding the inclusion criteria of participants (Table 5).Table 5Summary results of ERP study designs, organized by yearSourceFieldnMean age (SD)Diagnose confirmation toolsIQ assessmentInclusion criteriaMedicationASDTDASDTDTestCognitive standard scoresNo history ofASD: Mean (SD)TD: Mean (SD)DifferencesHearing LossVisualYes, if criteriaBorgolte et al. (2021)Audiovisual speech perception141540.3 (8.9)42.4 (12.7)Autism spectrum empathy quotientMWT-B108 (8)106.4 (5.5)ND–Yes–Chen et al. (2021)Phonetic encoding24247.60 (2.32)7.46 (1.91)ADOS-2Wechsler VIQ91.54 (14.65)100.13 (10.99)Yes–YesGARS-2Wechsler NVIQ99.33 (13.40)103.83 (10.50)NDDwyer et al. (2021)Heterogeneity: individual differences2439638.50 months (6.02)37.09 months (6.46)ADOS-GMSEL DQ65.25 (20.91)106.37 (11.58)–––ADI-RPiatti et al. (2021)Attentional orienting to sounds in speechASD/DD: 2217ASD/DD: 34.37 (7.11)38.21 (10.99) monthsADOS-2DQ score DD: < 71 > 71*––Included 1 participantASD/noDD: 12ASD/noDD: 39.62 (7.54)M-SELDQ score noDD: > 71Jamal et al. (2021)Sensory habituation1322Range 7.4–12.8Range 7.1–12.8ADOS-2WISC-V NVIQ104.42 (12.59)116.90 (9.73)ND–––SCQKadlaskar et al. (2021)Tactile and auditory reactivity patterns141410.13 (1.9)9.95 (1.36)ADOS-2Wechsler98 (21) verbal117 (11) verbalYes-***-*SP2DAS-II108 (18) non-verbal117 (16) non-verbalNDSRSDwyer et al. (2020)Heterogeneity: individual differences13281ADOS-GMSEL DQ64.83 (20.49)106.36 (11.57)–––ADI-RGreen et al. (2020)Speech sound differentiation1510ASD–LI: 7.38 (1.19)8.50 (1.72)CARS-2CELF-5ASD–LI: 98 (7.58)111.40 (11.61)*Yes––ASD + LI: 7.29 (1.70)ASD + LI: 61.57 (15.74)**Knight et al. (2020)Predictive coding21191415ADOS- 2Wechsler100117YesYesPsychotropic medication includedSchwartz et al. (2020)Own nameASD-V: 2727ASD-V: 17.21 (2.08)17.81 (3.00)ADOSLeiterASD-V: 109.63 (20.83)––Yes––ASD-MLV: 20ASD-MLV:16.81 (2.64)ASD-MLV: 54.75 (20.24)van Laarhoven et al. (2020)Predictive coding292918.64 (2.11)18.93 (1.22)ADOSWAIS- IV-NL103.03 (16.76)112.07 (11.68)NDYesYesYesDiStefano et al. (2019)Semantics401888.67 (22.04): VASD91.61 (24.50)SCQDAS-II Verbal IQ118.28 (16.19)75.97 (24.71) | 27.17 (14.32)***YesYes–92.42 (22.53): MVASDADOSDAS-II Non-Verbal IQ115.11 (16.50)86.52 (32.81) | 42.89 (19.69)**Grisoni et al. (2019)Semantic understanding and predictive coding202238 (10.3)31.9 (11.1)Autism Spectrum Quotient questionnaireLPS-3 Test119.5 (8.4)116.8 (9.5)NDYesYes-Patel et al. (2019)Prosody19 (12 M)20 (12 M)17.22 (6.30)14.99 (7.60)ADOS-2Wechsler98.11 (22.55)116.92 (13.44)**Yes––ADI-RRuiz‐Martínez et al. (2019)Habituation and auditory discriminative process16158.96 (1.01)8.86 (1.77)ADOS-GKBIT50.26 (38.99)85 (15.99)Yes––Thomas et al. (2019)Own name191352.29 (9.43)51.22 (9.05)ADOS-2MSEL verbal t-score36.08 (10.79)53.84 (7.34)YesYes–SCQMSEL non-verbal t-score36.04 (12.73)55.53 (8.00)Zhang et al. (2019)Non-Speech and Speech Pitch Perception161610.42 (2.12)9.48 (0.86) ~ Raven20.13 (2.50)21.13 (1.75)ND–––Arnett et al. (2018)Implicit language learning and receptive language ability277612.12 (2.9)13 (2.3)ADI-RDAS-II88.45 (28.55)113.59 (15.99)–––ADOS-2Charpentier et al. (2018)Prosody151510.0 (1.4)9.8 (1.4)ADI-RWechsler75 (29)118 (19)Yes–Included 4 participants161626.2 (6.8)26.2 (6.4)ADOS-295 (18)116 (16)Foss-Feig et al. (2018)Temporal silence gaps151711.86 (1.4)12.23(1.2)ADI-RWechsler118.27 (13.8)112.56 (12.6)NDYesYesYesADOS-2Intact cognitive skills (IQ > 70)Goris et al. (2018)Sensory Prediction Error1824AdultsAdultsADOSWAIS-III > 80 > 80NDHuang et al. (2018)Sensitivity to duration contrasts in speech and non-speech contexts22209.6 (1.88)9.4 (1.71)GARS-2Raven74 (23) tone103 (17) tone–––ADOS78 (15) vowel101 (16) vowelHudac et al. (2018)Cognitive response to environmental change1023112.29 (3.56)13.27 (2.34)ADI-RWechsler VIQ81.3 (30.58)115.06 (13.91)–––ADOS-2Wechsler NVIQ82.26 (30.08)115.71 (16.39)**Lindström et al. (2018)Prosody151610.410.1ICD-10WISC-III98 (12.89)108 (12.9)NDYes–YesLodhia et al. (2018)Auditory spatial cues151525.80 (6.81)27.07 (5.80)DSM-VWechsler122.93 (12.83)129.07 (7.40)NDYes–YesZhang et al. (2018)Lexical stress151610.04 (1.53)9.48 (0.86)EYABNon-verbal IQ––ND–––Bidet-Caulet et al. (2017)Voice perception161610 years 6 months(1 year 5 months)10 years 5 months (1 year 5 monthsADOS-GEDEI-R69 (25) verbalYes––ADI-RWISC85 (18) non-verbalGalilee et al. (2017)Detection and discrimination of speech and non-speech sounds141461 months (8.8)50 months (11)ADOS-GBAS-II verbal > 70 > 70NDYesYes–SCQWang et al. (2017)Speech-specific categorical perception161510.410.3GARS-2Raven83.7 (11.7)86.3 (6.61)NDYes––Karhson and Golob (2016)Top–down and bottom–up attentional processes121322.5 (4.1)22.8 (5.1)ADOSKBIT-2105.08 (19.25)101.25 (10.37)NDYes–YesADI-RRavenKey et al. (2016)Speech sound differentiation24186. 71 (1.34)7.14 (1.45)ADI-RK-BIT293.88 (17.41)110.44 (13.05)YesYes–ADOS-2Gonzalez-Gadea et al. (2015)Predictive coding241910.38 (1.97)11.63 (2.43)3DiRaven39.63 (9.83)40.16 (8.20)NDAll participants have no presence of known genetic condition other than ASD, or major psychiatric disorder (included in inclusion criteria for this systematic review)P1 pre-attentive perceptual processing, N2 stimulus detection, P3 stimulus categorization and memory updating, N400 semantics, P600 synaptic processing, MMN Mismatch negativity is the negative component of a waveform obtained by subtracting event-related potential responses to a frequent stimulus (standard) from those to a rare stimulus (deviant), SCQ Social Communication Questionnaire, ADOS-2 Autism Diagnostic Observation Schedule 2nd Editio, ADI-R Autism Diagnostic Interview-Revised, GARS-2 Gilliam Autism Rating Scale—Second Edition, KBIT-2 Kaufman Brief Intelligence Test—Second Edition, DAS-II Differential Abilities Scale—Second Edition, BAS-II British Ability Scales assessment, ASD/DD with developmental delay, ASD/noDD without developmental delay, MWT-B Mehrfachwahl–Wortschatz Intelligenz test, SNR − 16 dB, − 12 dB, − 8 dB noise conditions, ASD-LI ASD minus language impairment, ASD + LI ASD plus language impairment, Leiter Leiter-3 Standard Score, 3Di Diagnostic and Dimensional Interview, similar to ADI-R, SRS Social Responsiveness Scale-2, SP-2 Sensory Profile-2p < 0.05; **p < 0.01 (significant difference); ***p < 0.001 (significant difference)^#^Amplified 10 dB gain from voice input ~ = diagnose by the Education and Youth Affairs Bureau, which is a governmental and authoritative institution of Macau
Event-related potential waveforms have a series of positive and negative voltage deflections, referred by a letter indicating polarity (N, negative; P, positive) and a number indicating their latency in milliseconds (Luck and Kappenman 2012). As an example, N100 (also known as N1) indicates a negative polarity between 75 and 130 ms, usually associated with pre-attentive perceptual processing followed by P200 associated with stimulus detection (150–275 ms after stimulus presentation) (Key et al. 2005). Other components will be addressed in this review, such as P300 (P3; stimulus categorization and memory updating), N400 (semantics), and P600 (syntactic processing). Mismatch negativity (MMN) is the negative component of a waveform obtained by subtracting event-related potential responses to a frequent stimulus (standard) from those to a rare stimulus (deviant).
Some ASD studies have focused on early ERP components (Table 6), mainly showing reduced P1 latencies and amplitude (Patel et al. 2019; Arnett et al. 2018; Bidet-caulet et al. 2017). Looking particularly to patterns of auditory habituation, data suggest reduced habituation for ASD children in the P1 component and a decrease in MMN amplitude (Ruiz-Martínez et al. 2019). Pronounced habituation slopes have been observed for neurotypical subjects, with greatest difference at channel Fp1 and in the frontal and fronto-central electrodes (Jamal et al. 2020). For neurotypical subjects, P1 is stronger in the initial section of stimuli sequence, showing a gradual reduction in ERP amplitude over time (habituation) (Jamal et al. 2020). On the other hand, the ASD group shows absence of reduction between the first and last ERP, or even a positive slope toward the end of the experiment (reduced habituation) (Jamal et al. 2020). Regarding temporal processing with gap detection tasks, when compared with TD peers, ASD children with intact cognitive skills present reduced P2 amplitude (Foss-feig et al. 2018). The P2 component is associated with attention and stimulus classification, suggesting that the presence of a gap enhances the difficulty of primary level detection, and subsequent perceptual processes may fail to engage. In speech-in-noise tasks, high-functioning ASD adults present higher P2 amplitudes (Borgolte et al. 2021). These results suggest that the P2 component can be affected by the audiovisual process and specificities of both stimuli and condition. Early MMN (around 120 ms) show enlarged responses only for pure-tone context, with no other modulations dependent on action sound context (Piatti et al. 2021). Individual differences in auditory ERPs with four different loudness intensities (50, 60, 70, 80 dB SPL) (Dwyer et al. 2020) were tested using hierarchical clustering analysis based on ERP responses. It was possible to verify a pattern of linear increases in response strength accompanied by a disproportionately strong response to 70 dB stimuli for ASD young children, correlated with auditory distractibility (Dwyer et al. 2020). In a similar study, some clusters of ASD individuals presented weak or absent N2 by 60 dB and increased strength with higher intensities (70 or 80 dB) (Dwyer et al. 2021). However, there was an overlap between ASD and TD participants in several clusters (Dwyer et al. 2020, 2021), suggesting that sensory impairments in ASD might be largely accounted for the wide interindividual variability that exists within the spectrum.Table 6Summary results of ERP study results, organized by yearSourceFieldExperimentnMean age (SD); Range (min–max)Cognitive standard scoresParadigmStimulidB SPLResults ASDERP resultsASDTDASDTDDifferencesBorgolte et al. (2021)Audiovisual speech perceptionTemporal dynamics of speech-in-noiseVisual (lip movements) and auditory (voice) speech information that was either superimposed by white noise (condition 1) or not (condition 2)SNRWorse speech comprehension noise conditionHigher P2 amplitudes parietal141540.3 (8.9)42.4 (12.7)NDNo group differences in the NN condition, with a comprehension rate of nearly 100% in both groupsChen et al. (2021)Phonetic encodingVowel-speechFormant-exaggerated speech and non-speech70Enhanced P1 for vowel formant exaggeration in the TD group but not in the ASD groupFormant-exaggerated no P1 enhancement as TD24247.60 (2.32)7.46 (1.91)*Nonspeech similar P1 enhancement in both ASD and TD groupNDDifferences in neural synchronization in the delta-theta bands for processing acoustic formant changes embedded in non-speechDwyer et al. (2021)Heterogeneity: individual differencesListening of tones at four identity levelsSine waves of complex tones (sine waves of equal amplitude at different frequenciesVaried in intensity (50,60,70,80)Substantial heterogeneitySome weak or absent N2 negativities2439638.50 m (6.02)37.09 m (6.46)Hierarchical clusteringOverlap of ASD and TDOther N2 responses present at varying latenciesPiatti et al. (2021)Attentional orienting to sounds in speechPassive auditory oddball taskTwo deviant stimuli (one vowel sound and one complex tone) either in a speech or in a non- speech context60P3a mean voltages, we found an attenuated response in children ASD/noDD when deviant tones were presented in speech, but not in other conditions. Children with ASD/DD did not differ from TD in P3a mean voltagesMore negative MMN voltagesASD/DD: 2217ASD/DD: 34.37 (7.11)38.21 (10.99) mAttenuated P3a mean voltages ASD/noDD with deviantASD/noDD: 12ASD/noDD: 39.62 (7.54)Jamal et al. (2021)Sensory habituationVisual and auditory sequences of repeated stimuliAuditory: beep of 250 Hz; radial checkerboard on a gray background72Reduced habituation both auditory and visual stimuliNo reduction between the first and the last ERP13227.4–12.87.1–12.8NDRates of habituation correlated with several clinical scoresTD: negative slope; SD: positive slopeKadlaskar et al. (2021)Tactile and auditory reactivity patternsOddball paradigmSilent video while being presented with tactile and auditory stimuli60Differences in early perceptual processing of auditory (i.e., lower amplitudes at central region of interest), but not tactile, stimuliNo differences or later attentional componentsDwyer et al. (2020)Heterogeneity: individual differencesIdentify subgroups based on the normalized global field power (GFP) of their ERPs to auditory stimuli of four different loudness intensitiesSine waves of complex tones (sine waves of equal amplitude at different frequencies50, 60, 70, 804 clusters; Overlap of ASD and TDMore likely to display a pattern of relatively linear increases in response strength13281Disproportionately strong response to 70 dB stimuliAuditory disproportionately strong responses to 80 dBClusters did not differ in the chronological ages of their participants, which suggests that developmental changes in auditory evoked responses do not affect the loudness- dependency of overall response strength in the time-window of the present studyGreen et al. (2020)Speech sound differentiationMMN: auditory oddball speech and pure-tone sounds (ASD + LI vs ASD–LI vs TD)Stimuli matched for frequency, duration and intensity (Praat) + vowel (male speaker)70ASD were hypersensitive to soundsASD + LI: decreased MMN latency (left hemisphere) in response to novel vowel sound1510ASD–LI: 7.38 (1.19)0 (1.72)*Increased connectivity in primary sensory cortices at the expense of connectivity to association areas of the brainASD + LI: 7.29 (1.70)**Knight et al. (2020)Predictive codingPredictive coding in rhythmic tone sequences of varying complexityRepeated five-rhythm tones that varied in the Shannon entropy of the rhythm70No differences in the mechanisms of prediction error to auditory rhythms of varied temporal complexityASD + TD: decreased MMN21191415Schwartz et al. (2020)Own nameOne’s own name (OON) in cocktail scenarioQuiet and multispeaker setting80Auditory filtering disruptionTDs and ASD-Vs: significant MMRs to OON multisettingASD-V: 2727ASD-V: 17.21 (2.08)17.81 (3.00)–Strength of LPPs positively correlated with auditory filtering abilitiesASD-MLV: 20ASD-MLV:16.81 (2.64)van Laarhoven et al. (2020)Predictive codingPrediction errors in auditory prediction by visionUnexpected auditory omissions in a sequence of audiovisual recordings of a handclap in which the visual motion reliably predicted the onset and content of the sound61Unexpected auditory negative omission responseN1: similar for ASD and TD292918.64 (2.11)18.93 (1.22)NDDiStefano et al. (2019)SemanticsSemantic congruence ERPPictures were displayed followed by the auditory expected or unexpected word–EEG evidence of semantic processing, but it was characterized by delayed speed of processing and limited integration with mental representationsN400 effect with shorter latency in TD401888.67 (22.04): VASD91.61 (24.50)Late negative component present in TD, mid-frontal region in MVASD, not present in VASD92.42 (22.53): MVASDGrisoni et al. (2019)Semantic understanding and predictive codingBiological indicators of sound processing, (action-) semantic understanding and predictive codingauditory, passive listening, MMN task (sounds: action and non-action words—semantically congruent with regard to the body part they relate to or semantically incongruent or unrelated)–Deficits in predictive coding of sounds and words related to action, which is absent for neutral, non-action, soundsPrediction reduced for action202238 (10.3)31.9 (11.1)NDDeficits in semantic processingEarly MMN: enlarged for pure-tone context, no other modulation dependent on action sound contextPatel et al. (2019)ProsodyNeural basis of prosodic differencesPitch-perturbed auditory feedback paradigm during sustained vowel and speech production70 #Increased response onset latencies during sustained vowel productionReduced P1 amplitude19 (12 M)20 (12 M)17.22 (6.30)14.99 (7.60)**Ruiz-Martínez et al. (2019)Habituation and auditory discriminative processElectronic and human sounds (standard + deviant)Human and nonhuman sound Praat + standard tones 415 Hz65Lower auditory discriminationReduced habituation P116158.96 (1.01)8.86 (1.77)***Increased activation to repeatedly auditory stimulusDecrease in the amplitude MMNThomas et al. (2019)Own nameSubject’s own name in preschoolersSubject’s own name vs. unfamiliar nonsense name70Greater negativity to SON over frontal regionsN100 amplitude, SON negativity191352.29 (9.43)51.22 (9.05)******Zhang et al. (2019)Non-Speech and Speech Pitch PerceptionLexical tone contrasts and non-speech pitch variations + oddballLexical tone (e.g., /ga/)75Impaired ability when processing speech pitch informationNon-speech: NDTD: larger MMN responses (speech pitch contour) and stronger MMN (speech pitch height)161610.42 (2.12)9.48 (0.86)NDASD: more positive MMR (speech pitch height)Arnett et al. (2018)Implicit language learning and receptive language abilityArtificial language statistical learning taskTri-syllabic, artificial, unstressed (i.e., lacking prosodic cues) nonsense word combinations–Atypical lateralization of word-learningTD: attenuated P1 amplitude in the left hemisphere277612.12 (2.9)13 (2.3)**ASD: bilateral attenuationCharpentier et al. (2018)ProsodyProsodic change detectionVowel /a/ uttered by different female speakers with either neutral or emotional prosody (anger, fear, happiness, surprise, disgust, sadness70Change detection alteredDifferences between children and adults with ASDLarger P3a amplitude (P3a latencies shorter in adults)Earlier MMN151510.0 (1.4)9.8 (1.4)*161626.2 (6.8)26.2 (6.4)*Foss-Feig et al. (2018)Temporal silence gapsElectrophysiological response to silent gaps in auditory stimuliWhite noise (20 Hz–20 kHz) bursts + silent gaps80Degree of P2 amplitude attenuation was highly associated with clinical features, including more prominent sensory symptoms (i.e., auditory processing abnormalities and failure to register sensory input) and weaker processing language skillsReduced P2 amplitude151711.86 (1.4)12.23 (1.2)NDGoris et al. (2018)Sensory Prediction ErrorLocal prediction error processing is modulated by global context (i.e., global stimulus frequency)Oddball short sequences of either five identical sounds (local standard) or four identical sounds and a fifth deviant sound (local deviant)70ASD: less flexible in modulating their local predictionsMMN modulated by global smaller effect in ASD1824AdultsAdultsNDNo differences P3bHuang et al. (2018)Sensitivity to duration contrasts in speech and non-speech contextsOddball paradigmPure tone + vowel60Distinct patterns of discrimination and orienting responsesPure-tone: diminished response amplitudes and delayed latency MMN; ND P3a22209.6 (1.88)9.4 (1.71)Vowel: smaller P3a;: ND MMNHudac et al. (2018)Cognitive response to environmental changeProcessing and habituation to deviance soundSilent video of a trip to the zoo while passively attending to randomly presented frequent tones (70%) + infrequent tones (15%) + novel sounds (15%)65Overall heightened sensitivity to changeGreater P3a amplitude to novel sounds1023112.29 (3.56)13.27 (2.34)Auditory oddball taskYouth: slower attenuation of the N1 response to infrequent tones and P3a response to novel soundsLindström et al. (2018)ProsodyBehavioral sound-discrimination natural word stimuli uttered with different emotional connotations(neutral, sad, scornful and commanding)56Anomalous neural prosody discriminationDifferentially distributed on the scalpDiminished amplitude of P3a151610.410.1NDImpaired orienting to prosodic changesSluggish perceptual prosody discrimination in children with ASDLodhia et al. (2018)Auditory spatial cuesSpatial cues to auditory object formation – the relative timing and amplitude of sound energy at the left and right earsDichotic pitch stimuli – white noise stimuli in which interaural timing or amplitude differences applied to a narrow frequency band of noise typically lead to the perception of a pitch sound that is spatially segregated from the noise70ASD: object-related negativity to amplitude cuesP400 missing151525.80 (6.81)27.07 (5.80)NDDo not experience a general impairment in auditory object formationLater attention-dependent aspects of auditory object formation missingBidet-Caulet et al. (2017)Voice perceptionVocal (speech and non-speech) and non-vocal soundsVocal and non-vocal sequences70ASD: lack of voice-preferential responseTD: voice-sensitive response over right fronto-temporal161610 y 6 m (1 y 5 m)10 y 5 m (1 y 5 m)ASD: atypical response to non-vocal soundsSmaller P100 non-vocal soundsSmaller right fronto-temporal negative Tb peak non-vocal soundsGalilee et al. (2017)Detection and discrimination of speech and non-speech soundsNovel paired repetitionPairs of stimuli (speech sounds, non-speech sounds)60Speech versus non-speech detectionN330 match/mismatch responses right hemisphere141461 m (8.8)50 m (11)NDAtypical speech versus non-speech processingAbsent effect of match/mismatch 600 ms for non-speech followed by speechWang et al. (2017)Speech-specific categorical perceptionDistinct pitch processing pattern for speech and non-speech stimuli and speech-specific deficit in categorical perception of lexical oddball paradigmPitch deviations representing within-category and between-category differences in speech and non-speech contexts75Lack of categorical perception in the lexical tone conditionEnhanced within-category MMRs161510.410.3NDSpeech-specific categorical perception deficitZhang et al. (2018)Lexical stressOddball neural responses bilingual children in L2 lexical stressMOther (1st syllable stressed) vs. moTHER (deviant)–Chinese-English bilingual ASD: less sensitive to lexical stressReduced MMN amplitude (left temporal- parietal)151610.04 (1.53)9.48 (0.86)NDMore negative MMN response for ASD (right central-parietal, temporal-parietal, and temporal sites)ASD: right hemisphere more activatedKarhson and Golob (2016)Top-down and bottom-up attentional processesOddball target detectionTarget, non-target, and distractor60TD: top–down control (P3b latency) increased under greater load in controlsASD: ND P3a121322.5 (4.1)22.8 (5.1)NDEnhanced bottom-up processing of sensory stimuli in people with autismEarly ERP responses (P50 amplitude) positively correlated to increased sensory sensitivityKey et al. (2016)Speech sound differentiationContrasting consonant–vowel syllables during a passive listening paradigmSix syllables /ba/, /da/, /ga/, /bu/, /du/, and /gu/75Reduced consonant differentiation84- to 308-ms period24186. 71 (1.34)7.14 (1.45)Related to individual differences in non-verbal versus verbal abilitiesND: 432–700 and 320- to 444-ms intervalGonzalez-Gadea et al. (2015)Predictive codingDescribe mechanisms responsible for attentional abnormalitiesStandard and deviant tone sequences (expected and unexpected)–Top-down expectation abnormalities could be attributed to a disproportionate reliance (precision) allocated to prior beliefs in ASDReduced superior frontal cortex (FC) to unexpected events241910.38 (1.97)11.63 (2.43)NDAssociated with specific control inhibitory controlIncreased dorsolateral prefrontal cortex (PFC) activation to expected eventsAll participants have no presence of known genetic condition other than ASD, or major psychiatric disorder (included in inclusion criteria for this systematic review)P1 pre-attentive perceptual processing, N2 stimulus detection, P3 stimulus categorization and memory updating, N400 semantics, P600 synaptic processing, MMN mismatch negativity is the negative component of a waveform obtained by subtracting event-related potential responses to a frequent stimulus (standard) from those to a rare stimulus (deviant), SCQ Social Communication Questionnaire, ADOS-2 Autism Diagnostic Observation Schedule 2nd Edition, ADI-R Autism Diagnostic Interview-Revised, # amplified 10 dB gain from voice input, GARS-2 Gilliam Autism Rating Scale—Second Edition, KBIT-2 Kaufman Brief Intelligence Test—Second Edition, *DAS-II * Differential Abilities Scale—Second Edition, BAS-II British Ability Scales assessment, ASD/DD with developmental delay, ASD/noDD without developmental delay, MWT-B Mehrfachwahl–Wortschatz Intelligenz test, ASD-LI ASD minus language impairment, ASD + LI ASD plus language impairment, Leiter Leiter-3 Standard Score, 3Di Diagnostic and Dimensional Interview, similar to ADI-RP < 0.05; **P < 0.01 (significant difference); ***P < 0.001 (significant difference)SNR = − 16 dB, − 12 dB, − 8 dB noise conditions ~ = diagnosed by the Education and Youth Affairs Bureau, which is a governmental and authoritative institution of Macau
A large-scale study tested 133 children and young adults in an auditory oddball task, comparing mismatch negativity and P3a results, as well as temporal patterns of habituation (N1 and P3a) (Hudac et al. 2018). The P3a component is indexed by different levels of attentional orienting. Results showed heightened sensitivity to change to novel sounds in ASD subjects, increased activation upon repeated auditory stimuli, and dynamic ERP differences driven by early sensitivity and prolonged processing (Ruiz-Martínez et al. 2019; Hudac et al. 2018). To test the neural indices of early perceptual and later attentional factors underlying tactile and auditory processing, ASD and age- and non-verbal IQ-matched TD peers were compared (Kadlaskar et al. 2021). Using an oddball paradigm where children watched a silent video while being presented with tactile and auditory stimuli, results showed reduced amplitudes in early ERP responses for auditory stimuli but not tactile stimuli in ASD children. The differences in neural responsivity were associated with social skills (Kadlaskar et al. 2021). Regarding top–down and bottom–up attentional processes, young ASD children with no developmental delay seemed to present more negative MMN voltages and an attenuated response of P3a mean voltages when deviant tones were presented in speech (Piatti et al. 2021). When compared with TD peers, bilingual children with ASD seemed to be less sensitive to lexical stress, with reduced MMN amplitude at the right central–parietal, temporal–parietal, and temporal sites (Zhang et al. 2019). Children with developmental delay did not differ from the control group in the P3a component (Piatti et al. 2021). Compared to adults, there was enhanced bottom–up processing of sensory stimuli in participants with high-functioning autism, with early ERP responses positively correlated to increased sensory sensitivity (Xiaoyue et al. 2017). In ASD children, more positive MMR was observed in the processing of speech pitch height (Zhang et al. 2019), suggesting hypersensitivity to higher frequency tones.
Another relevant feature for auditory processing is prosody, the rhythmic and intonational aspect of language. Event-related potential (ERP) studies show preserved processing of musical cues in ASD individuals, but with prosodic impairments (Depriest et al. 2017). Differences in prosody such as intonation are highly relevant for language-related impairments in ASD with a significant impact on communication. To test prosodic processing, many studies record brain responses to neutral and emotional prosodic deviances reflecting change detection (MMN) and orientation of attention toward change (P3a).
Children with ASD present atypical neural prosody discrimination, with distinct patterns depending on the experimental design. For instance, the P3a component becomes more prominent upon greater difference of stimulus change. Studies using sound-discrimination tasks with lexical tone contrasts based on naturally produced words (e.g., a vowel with neutral or emotional prosody such as sadness) show different P3a depending on the IQ level of ASD children. A study with high-functioning ASD children shows diminished amplitude of P3a (Lindström et al. 2018). In a study comparing children and adults, low-functioning children revealed a larger P3a compared to the control, with P3a latencies shorter in ASD adults (Charpentier et al. 2018). Regarding change detection, ASD adults presented an earlier MMN (Charpentier et al. 2018). Both results suggest atypical neural prosody discrimination and deficits in pre-attentional orientation toward any change in the auditory environment (Lindström et al. 2018; Charpentier et al. 2018). When vowel and pure tone are compared within tone languages (smaller physical difference between standard and deviants compared to non-tone languages), ASD children still presented diminished response amplitudes and delayed latency of MMN for pure tones, and smaller P3a for vowel (Huang et al. 2018). At a pre-attentive perceptual processing level, low-functional ASD children present increased response onset latencies during sustained vowel production, with reduced P1 ERP amplitudes (Patel et al. 2019; Bidet-caulet et al. 2017; Charpentier et al. 2018), lacking neural enhancement in formant-exaggerated speech tasks (Chen et al. 2021). When a non-speech sound is followed by a speech sound, TD children present match/mismatch effects at approximately 600 ms, as opposite to ASD (Galilee et al. 2017). Interestingly, when speech and non-speech sounds are compared between high-functioning ASD children matched on age, gender, and non-verbal IQ with TD group, ASD children show impaired processing ability regarding speech pitch information, but no differences are observed for non-speech sounds (Zhang et al. 2019; Chen et al. 2021). Regarding speech differentiation, there seems to be no differences in voice perception. Low-functioning children with ASD seem to present atypical response to non-vocal sounds (Bidet-caulet et al. 2017), with atypical consonant differentiation in the 84- to 308-ms period, related to individual differences in non-verbal versus verbal abilities (Key et al. 2016).
There is EEG evidence for altered semantic processing in children with ASD, characterized by delayed processing speed and limited integration with mental representations (Piatti et al. 2021; Distefano et al. 2019). Semantic processing refers to encoding the meaning of a word and relating it to similar words or meanings. During passive and active listening, there is a pre-attentive stage of sound segregation. When individuals attend to auditory stimuli, there are some components that can distinguish the stage of neural processes. The Subject’s own name (SON) is a unique auditory stimulus for triggering an orienting response. Sounds need to stand out from the background to elicit an orienting response. SON is automatically distinguished from other names without reaching awareness, causing involuntary attention take (Tateuchi et al. 2015). Children with ASD present the ability to selectively respond to one’s own name with greater negativity over frontal regions, reflecting early automatic pre-attentive detection (Thomas et al. 2019), when compared with TD peers. After the pre-attentional level, there is an orienting response to cause a shift of attention, where the auditory system makes use of amplitude and timing cues to differentiate sounds from different spatial locations, giving them context. Although high-functioning adults with ASD do not seem to have general impairment in auditory object formation, they seem to display alterations in attention-dependent aspects of auditory object formation (P400 missing) (Thomas et al. 2019), as well as disruption of auditory filtering (Huang et al. 2018). These deviations at top–down processing might be linked with deficits in perceptual decision-making.
Some studies highlight the importance of proper ability to anticipate upcoming sensory stimuli. ASD adults seem to be less flexible than controls in the modulation of their local predictions (Goris et al. 2018), affecting their function of global top–down expectations. Adults diagnosed with ASD present deficits in predictive coding of sounds and words in action–sound context, with no deficits in predictive coding for neutral, non-action, and sounds (Grisoni et al. 2019; Laarhoven et al. 2020). When using varied auditory rhythms, both ASD and TD presented decreased MMN, with no difference in error prediction (Knight et al. 2020).
There are some interesting data regarding cognitive function lateralization in children with ASD. When comparing ERP responses for speech and non-speech sounds, speech-related events where only detected over temporal electrodes in the left hemisphere (Galilee et al. 2017), compared to bilaterally N330 match/mismatch responses in neurotypical children (Galilee et al. 2017). Regarding ASD children with impairments specifically at language level, results show hypersensibility to sounds with decreased MMN latency at the left hemisphere (Green et al. 2020). Older children with non-verbal IQ impairments presented bilateral attenuation in a word-learning task, as opposed to attenuated P1 amplitude present in the left hemisphere of TD children (Arnett et al. 2018). Young children with high-functioning ASD seem to fail to activate right-hemisphere cognitive mechanisms, probably associated with social or emotional features of speech detection.
Impairments at the level of emotional perception can be related to internal distractions or overload of sensory information that hinder social communication. Studies using sympathetic skin response show that children diagnosed with ASD exhibit delayed habituation to auditory stimuli (Bharath et al. 2021). The predominant state of sympathetic nerves can affect the predisposition to filter and perceive cues, and also influence anxiety levels or valence of social cues. Individuals with ASD seem to present higher levels of perceptual capacity, which might be correlated with higher levels of sensory sensitivity (processing more information at any one time) (Brinkert and Remington 2020).
Emotional expressiveness is highly important for emotional perception, carrying non-verbal information that helps forming social judgments, and predisposing individuals for further social engagement. A study focusing on emotion recognition in intellectually disabled children with ASD found that these children displayed poorer performance in recognizing surprise and anger in comparison to happiness and sadness (Golan et al. 2018). A different study tested emotion performance by comparing ASD children with siblings without ASD diagnosis and TD peers (Waddington et al. 2018). Interestingly, the authors found not only poorer emotion performance in terms of speed and accuracy in the ASD group, but also poorer performance in the ASD sibling group compared to TD controls (Waddington et al. 2018), suggesting a possible contextual influence in emotional perception.
Children with ASD seem to present lower autonomic reactivity to human voice, with impairments in the vocal emotion recognition tests, albeit normal pro-social functioning (social awareness and social motivation) (Anna et al. 2015; Schelinski and Kriegstein 2019). This interesting result raises the question whether social impairments in ASD could be a consequence of hyperarousal from sensory overload.
Regarding other assessment paradigms, children with ASD seem to struggle with face-to-face matching, when compared to voice-face and word-face combinations (Golan et al. 2018), with worst performance in noisy environments (Newman et al. 2021). The ability to integrate facial-voice cues seems to be correlated with socialization skills in children with ASD (Golan et al. 2018).
Together, these studies highlight the importance of reappraising cognitive function in light of the sensory systems, such as the auditory the Peripheral Auditory System, where auditory pathway starts, as well as the Central Auditory Nervous System, where all auditory information gets integrated and processed.
Sounds are produced by acoustic waves that reach the external auditory canal and travel to the eardrum causing vibration of the tympanic membrane at specific frequencies (the typical hearing frequency range in humans is 20 to 20.000 Hertz, cycles per second) (Peterson et al. 2022). The vibration of the tympanic membrane causes vibration of tiny bones in the middle ear that amplify the signal and send it to the cochlea. The signal travels to fluid-filled sections of the cochlea, the scala vestibuli and the scala tympani, and oscillations of these sections transmit energy to the scala media, causing shifts between the tectorial and basilar membrane. The basilar membrane contains receptor hair cells that can be either activated or deactivated by shifts that open or close potassium channels. Cells near the base of the cochlea respond to high frequencies, with increased flexibility to respond to lower frequencies toward the apex of the cochlea (Peterson et al. 2022; Zhao and Müller 2015; Delacroix and Malgrange 2015). Inner hair cells are responsible for the majority of auditory processing. Outer hair cells synapse only on 10% of the spiral ganglion neurons (Delacroix and Malgrange 2015). Neurons within the spiral ganglion mostly synapse at the base of hair cells to the auditory nerve (cochlear nerve). The cochlear nerve then sends up information to the brain cortex through a serious of nuclei in the the cochlear nuclei (medulla), superior olivary complex (pons), lateral lemniscus (pons), inferior colliculus (midbrain), and medial geniculate nucleus (midbrain) (Felix et al. 2018). Although the primary auditory pathway mostly ascends to the cortex through the contralateral side of the brainstem, all levels of the auditory system have crossing fibers, receiving and processing information from both the ipsilateral and contralateral sides (Peterson et al. 2022).
Reported cognitive deficits in ASD regarding speed and accuracy of sound stimuli assessment (Distefano et al. 2019; Waddington et al. 2018) might potentially be contributed by impairments in impulse initiation at the cochlear nerve, or impairments in the transmission and conduction of signals along the brainstem, as it occurs in demyelinating diseases. One tool used to measure neural functionality of the auditory brainstem is the auditory brainstem response (ABR) (Celesia 2015; Jewett and Williston 1971). Participants usually perform hearing screenings to exclude hearing disabilities, such as lesions below or within the cochlear nuclei. Of note, since 2015, there are few experimental studies assessing the integrity of the peripheral auditory system in ASD.
The auditory brainstem response (ABR) measures electrical signals associated with the propagation of sound information through the auditory nerve to higher auditory centers, after an acoustic stimulus. Major alterations in neuronal firing along this pathway can be detected as changes in auditory brain response ([99]). Complementary to the use of a short click as a classical acoustic stimulus, ABR is also often performed with complex sounds, such as syllables, which incorporate an array of complexity more similar to speech. Two major categories of ABR stimulus are detailed click-ABR and speech-ABR.
Most ABR studies report differences in auditory brainstem processing for ASD individuals when compared with control groups (Table 7). Results are discussed taking into consideration the age of participants and different time-points, their cognitive pattern, type of stimuli, and experimental design.Table 7Summary of publications sources used in this systematic review, related with ABR, organized by yearSourceStimuliCountrynMean age (SD)ASD confirmation toolsTimepointsASDTDASDTDDelgado et al. (2021)CUSA370 (286 M)128,181 (63882 M)1.74 (2.93) d1.80 (2.98) dDSM-V2Fujihira et al. (2021)CJapan17 (15 M)20 (17 M)30.5 (4.7)29.3 (3.9)DSM-V1IQ > 85ElMoazen et al. (2020)CEgypt20 (16 M)20 (16 M)4.99 (2.59)5.02 (2.64)DSM-V1Jones et al. (2020)C + SUSA18 (13 M)18 (13 M)2.941 (0.45) y3.058 (0.35) yADOS1Tecoulesco et al. (2020)C + SUSA12 (11 M)12 (10 M)19.90 (1.20) m30.93 (5.87) mADOS2Claesdotter-Knutsson et al. (2019)CSweden39 (18 M)34 (23 M)11.50 (3.0) y (M)13.18 (3.2) y (M)ADOS112.71 (3.36) y (F)13.12 (3.47) y (F)Chen et al. (2019)SChina15 (12 M)20 (14 M)4.86 (1.48) y4.57 (0.53) yGDDS2CARSRamezani et al. (2019)SIran28 (28 M)28 (28 M)14.36 (1.86) y14.99 (1.92) yDSM-V1IQ > 85S speech-ABR, C click-ABR, M male, ASD autism spectrum disorder, TD typical development, y years, m months, d days, F female, M male
In the first 10 ms after a click, click-ABR produce five-to-seven waveforms (wave I–VII). These wave peaks reflect the propagation of electrical activity as it travels along the auditory pathway, providing information in terms of latency (speed of transmission), amplitude of the peaks (interpreted as the number of neurons firing), inter-peak latency (time between peaks), and interaural latency (correlation between left and right ear) (Musiek and Lee 1995).
Some studies with click-ABR (Table 8) show longer latencies for ASD participants in wave V, and longer latency of inter-peak intervals in waves I–V and III–V (Tecoulesco et al. 2020; Jones et al. 2020). However, these experiments were done with toddlers. Interestingly, a recent study tested older children in a click-ABR paradigm (Claesdotter-Knutsson et al. 2019). Results do not show differences in ABR latency, but reveal a higher amplitude of wave III in ASD, suggesting functional alterations at the pons region (Claesdotter-Knutsson et al. 2019). This experiment used binaural sound exposure, showing a higher degree of correlation between left and right ear in the ASD group. A different study found absence of asymmetry in the latency of wave V between the right and left sides, both in ASD and control groups (ElMoazen et al. 2020). The authors further report a reduced amplitude in the binaural interaction component in younger children with ASD, which might reflect reduced binaural interaction at younger ages not related to artificial latency shift (ElMoazen et al. 2020). A recent study looking at newborns later diagnosed with ASD at the age of 3–5 years showed ABR latency delays (Delgado et al. 2021), suggesting the emergence of differences in acoustic processing, at the brainstem level, right after birth. A more recent study tested adults with ASD and found no differences in absolute ABR wave latencies (Fujihira et al. 2021). The authors showed a shorter summating potential (SP), suggesting normal auditory processing in the brainstem for ASD adults (Fujihira et al. 2021).Table 8Summary results using click-ABR and speech-ABR, organized by yearSourceStimulidB SPLMaterialSoundLatencyAmplitudeOther measuresASDASDASDDelgado et al. (2021)Click35 nHLEarphonesRight, leftDelayedNFT1: greater newborn ABR phase valuesT2: slower neurological responsesFujihira et al. (2021)Click100(67.9 nHL)EarphonesRight earShorter SPNFElMoazen et al. (2020)Click65 nHLHeadphonesRight, Leftlonger BICReduced BICNo asymmetry in the latency of wave V between the right and left side in both groupsBinaurallyDelay at wave VJones et al. (2020)Click98.5EarphonesRight earLonger interpeaks waves I–V; III–VNDNo differences between auditory processing and behavioral measuresSyllable /da/80Higher in wave OTecoulesco et al. (2020)Click80EarphonesRight earLonger wave VNDStability of similar developmental patternsSyllable /da/80NDClaesdotter-Knutsson et al. (2019)Click80HeadphonesBinaurallyNDHigher wave IIIHigher degree of correlation between left and right earChen et al. (2019)Syllable /da/80HeadphonesRight earT1: prolonged in wave V, AT1: smaller in wave EPositive correlation between wave A amplitude and GDDS language scoreT2: prolonged in wave FT2: prolonged in wave FT1—> T2: shorted wave VT1—> T2: increased wave A, CRamezani et al. (2019)Syllable /da/80EarphonesRight earLonger in wave V, A, D, E, FNDShorter SNRLonger V-ALonger RMS amplitudeNote: only wave V was detected in newbornsdB SPL* decibel sound pressure level, T1 timepoint1, T2 timepoint2, ND no differences, SNR obtained from the mean amplitude of the response divided by the mean amplitude of the pre-stimulus activity, SP summating potential, NF not referred, BIC binaural interaction component
The most common speech-ABR stimulus used is the universal syllable/da/. After the stimulus, a subcortical response emerges as an ABR waveform of seven peaks (V, A, C, D, E, F, O). Peaks can reflect either a change in the stimulus (i.e., onset, offset, or transition) or the periodicity of the stimulus. There are two main components in speech-ABR: the onset response (waves V and A) and the frequency-following response (FFR; waves D, E, and F). The wave C represents the consonant–vowel transition, while the wave O represents the end of the vowel. Analysis of FFR includes measurements of response timing (peaks), magnitude (robustness of encoding of specific frequencies), and fidelity (comparison of FFR consistency across sessions, which gives an index of how stable the FFR is from trial to trial (Krizman and Kraus 2019)).
Similarly to click-ABR, speech-ABR studies (Table 8) also show longer latencies for ASD participants, including high-functioning ASD individuals (Ramezani et al. 2019). Recently, a longitudinal study included two assessment time-points (interval of 9.68 months) to look for longitudinal changes in speech-ABR (Chen et al. 2019). No differences were found in the TD group, whereas differences were found in the ASD group (shorter latency wave V and increased amplitude wave A and C), suggesting an age effect for ASD (Chen et al. 2019). Another study had two assessment time-points to investigate neural response stability, a metric measured by trial-by-trial consistency in the neural encoding of acoustic stimuli (Tecoulesco et al. 2020). Results showed that children with a more stable neural encoding of speech sounds, in both groups ASD and TD, demonstrated better language processing at a phonetic discrimination task (Tecoulesco et al. 2020). Individuals’ performance was assessed in a different study through listening structured and repetitive listening exercises, with increasing difficulty levels (Ramezani et al. 2021). Results showed gradual improvement in ASD individuals’ temporal auditory skills (Ramezani et al. 2021).
A relevant association has been found between sensory overload and behavioral measures in ASD, but without relevant auditory processing association (Font-Alaminos et al. 2020). For children with ASD, the FFR signal has been described as unstable across trials (Otto-Meyer et al. 2018), tending to increase with stimulus repetition (Font-Alaminos et al. 2020), which suggests an unstable neural tracking at the level of subcortical auditory system (Table 9). The development pattern of auditory information processing was assessed in preschool children with ASD (Chen et al. 2019). Results show a positive correlation between wave A and Gesell Developmental Diagnosis Schedules (GDDS) language score (Chen et al. 2019). According to authors, the latency between V and A complex could suggest a weakened synchronization of neural response at the beginning of speech stimulus (Chen et al. 2019). A different study also revealed longer latencies of the transient FFR components (which include D, E, and F, ABR waves) in the ASD group (Ramezani et al. 2019). These results suggest a possible disturbance in brain pathways implicated in FFR generation [the direct pathway to the contra-lateral IC via the lateral lemniscus, and the ipsilateral pathway via superior olivary complex and the lateral lemniscus (Ramezani et al. 2019)] further raising the question whether this could be a potential compensatory mechanism in ASD.Table 9Summary results testing FFR, organized by yearSourceStimulidB SPLStudySoundResultsnMean age (SD)Cognitive standard scoresASDASDTDASDTDMean (SD)Font-Alaminos et al. (2020)AM pure tones75Ability to filter out auditory repeated informationRightIncrease of FFR with stimulus repetition17189.1 (1.7)8.8 (1.9)IQ ≥ 100Roving-frequency paradigmRelated with sensory overloadOtto-Meyer et al. (2018)Click + syllable60–80Neural stability in response to soundRightLess stable FFRs to speech sounds reduced auditory stability121210.71 (2.07)IQ ≥ 80Voiced with a flat pitchAM Amplitude-modulated
The integrity of the peripheral auditory system can also be evaluated using otoacoustic emissions (OAEs). Evoked otoacoustic emissions are produced by healthy ears in response to an acoustic stimulus delivered into a sealed ear canal. The acoustic stimulus causes basilar membrane motion which triggers an electromechanical amplification process by the cochlear outer hair cells, producing a sound that echoes back into the middle ear (otoacoustic emissions). These nearly inaudible emissions are measured using a sensitive microphone and help evaluate normal cochlear function. A study tested a group of children and adolescents with ASD (ASD with Full-Scale IQs higher than 85) with normal audiometric thresholds (Bennetto et al. 2016). Results showed that children with ASD presented reduced OAEs at 1 kHz frequency range, with no differences outside this critical range (at 0.5 and 4–8 kHz regions) (Bennetto et al. 2016), thus suggesting reduced outer hair cell function at 1 kHz. Outer hair cells synapse directly with neurons originating in the nuclei of the superior olivary complex. A morphological post-mortem study of subjects with ASD showed significantly fewer neurons in the Medial Superior Olive (MSO), a specialized nucleus from the superior olivary complex (Mansour and Kulesza 2020). Results also showed that the existing fewer neurons in the MSO are smaller, rounder, and with abnormal dendritic orientations (Mansour and Kulesza 2020). However, the small sample size, variability of post-mortem tissue origin and quality (7 post-mortem samples from drowning, seizure, or other death causes), may hinder conclusions from this study. Previously, a different study found no evidence regarding asymmetrical or reduced middle ear muscle (MEM) reflexes and binaural efferent suppression of transient evoked otoacoustic emissions responses (Bennetto et al. 2016). However, a more recent study showed OAE asymmetry, with the medial olivocochlear system being apparently more effective in the right than the left ear in ASD (Aslan et al. 2022).
ASD is a neurodevelopmental disorder with behavior and cognitive traits associated with atypicalities in the central nervous system (CNS). Integrity of the central nervous system can be assessed experimentally by several techniques, such as magnetoencephalography (MEG; Table 10), magnetic resonance imaging (MRI; Table 11), as well as other multimodal tools (Table 12).Table 10Summary of publications sources using MEG, organized by yearExperimentnMean age (SD)SourceMethodStudyParadigmStimuli/measuresResultsCognitive standard scoresor Mean age (min range- max range)Relevant resultsASDTDASDTDYoshimura et al.(2021)MEGP1mBilateral auditory cortical response (P1m)Sinusoidal pure tonesASD: shorter P1m latency in the left hemisphereMental Processing Scale: TD > ASD 294674.7 (10.8) m70.3 (5.9) mCorrelation between P1m latency and language conceptual abilityMatsuzaki et al. (2020)MEGM50 and M100: comparison between children and adolescentsSignals left and right superior temporal gyrusAuditory presentation of tonesASD: Delayed M50 and M100 latenciesND: IQ (mean) > 10058 children36 children10.07 (2.38)9.21 (1.6)Differences in M50 and M100 persisted in adulthoodND: IQ (mean) > 10019 adolescents19 adolescents23.80 (6.26)26.97 (1.29)Ono et al. (2020)MEGASSRAssessing neural synchrony at specific response frequenciesASSR at 20 Hz and 40 HzASD + TD: Responses to 20 Hz and 40 Hz detectedTD > ASD233274.8 (11.2) m69.7 (6.2) mASD + TD: right dominance of the 40-Hz ASSRTD: right-side 40-Hz ASSR was correlated with ageSeymour et al. (2020)MEGASSRs + tGBRReplicate and extend findings regarding reductions in ASSRs at 40 Hz1.5 s-long auditory clicktrain stimulusASSRs: bilateral primary auditory regionsND: Raven score >40181816.67 (3.2)16.89 (2.8)ND for tGBR from 0-0.1 s following stimulusASD: reduced oscillatory power at 40 Hz from 0.5 to 1.5 s post-stimulus onset, for both left and right A1ASD: reduced inter-trial coherence (phase consistency over trials) at 40 Hz from 0.64-0.82 s for right A1 and 1.04-1.22 s for left A1Stroganova et al. (2020)MEGPitch processingSpectrally complex periodic sounds (ASSR + SF)Investigate the ASSR and SF evoked by monaural 40 Hz click trainsSF and ASSR: dominated in the right hemisphereASD < TD 35379.69 (1.5)10.08 (1.5)SF and ASSR: higher in the hemisphere contralateral to the stimulated earASSR: ASSR increased with age both groupsSF: moderately attenuated in both hemispheres ASDSF: markedly delayed and displaced in the left hemisphere (ASD boys)Wagley et al. (2020)MEGPredictive processing with naturalistic statistical learning taskSpeech neural signals of statistical learningEvoked neural responses to syllable sequences in a naturalistic statistical learning corpus - left primary auditory cortex, pSTG, IFG, across three repetitions of the passageTD: neural index of learning in all three ROIs measuredIQ TD > (ASD) > 90 151410.06 (1.47)10.00 (1.64)TD: change in evoked response amplitude as a function of syllable surprisal across passage repetitionsTD: surprisal increased -> amplitude of the neural response increased (after repeated exposure)ASD: did not show this pattern of learningMatsuzaki et al. (2019a)MEGMMFMMF delays in extremely language impaired ASDMFF responses bilaterally during an auditory oddball paradigm with vowel stimuliASD-MVNV: bilaterally delayed MMF latenciesCELF CLI >85; “ASD-V“ASD-VASD-LIASD-MVNV27ASD-VASD-LIASD-MVNVdelayed MMF responses associated with diminished language and communication skillsCELF core language index <85; “ASD-LI”2721910.55 (1.21)10.67 (1.21)9.67 (1.41)10.14 (1.38)TD: leftward lateralization of MMF amplitudeASD-MVNV and verbal ASD: abnormal rightward lateralizationRoberts et al. (2019)MEGM50 and M100: study with ASD-MVNV and ASD-VSignals left and right superior temporal gyriTone stimuliASD-MVNV: delayed M50 and M100 latencies, greater than ASD-VFull-Scale IQ: TD > ASD-VASD-VASD-MVNV34ASD-VASD-MVNV10.18 (1.36)Latencies were associated with language and communication skillsNon-verbal IQ: TD > ASD-V > ASD-MVNV551610.64 (1.31)9.85 (1.32)Brennan et al. (2019)MEGPredictive processing with naturalistic languagePredictive sentence comprehension during story-listeningListen to an audiobook storyPredictive parsing equivalent between high-functioning individuals with ASD and TD peersND: IQ (mean) > 10014139.49.8Neuromagnetic signals correlated with word-by-word statesVERBAL: TD > ASDLinguistic prediction in school-aged childrenMatsuzaki et al. (2019b)MEGMMFMMF and auditory language discrimination of vowel stimuliAuditory oddball paradigm with vowel stimuli (/a/ and /u/).ASD: MMF delayedND: IQ (mean) > 10091622.22 (5.74)27.25 (6.63)ASD: earlier M100 component to single stimulus tokens delayedNo correlation between delayed M100 and MMFTD: leftward lateralization of MMF amplitudeASD: rightward lateralization MMF amplitudeLambrechts et al. (2017)MEGInterval timingProcessing of duration as compared to pitchComparison of two consecutive tones according to their duration or pitchASD: less able to predict the duration of the standard tone accuratelyND: IQ (mean) > 100181825:3 (8:1)25:3 (8:1)Engage less resources for the Duration task than for the Pitch task regardless of the contexty:my:mLower sensitivity for duration discrimination behaviourally in ASDASD adults are less able to predict the offset of a standard toneDemopoulos et al. (2017)MEGAuditory and Somatosensory Cortical ResponsesIndices of auditory and somatosensory cortical processingMagnitude of responses to both auditory and tactile stimulationASD: delayed M200 latency response from the left auditory cortexIQ (mean) TD > ASD > 100**18199.82 (1.17)9.79 (1.11)ASD: delayed somatosensory responseASD: left M200 latency delay was significantly associated with performance on the WISC-IV Verbal Comprehension IndexCortical auditory response delays were not associated with somatosensory cortical response delays or cognitive processing speedMamashli et al. (2017)MEGAuditory Processing in NoiseCortical responses with passive mismatch paradigm.Paradigm 1) in a quiet background, 2) in the presence of background noiseQuiet common neural sources of the MMF response in both groups (RTG + IFG)Verbal IQ: ND191713 (3)12 (2)Temporal and frontal cortical locations, and functional connectivity with spectral specificity between those locationsNoise MMF response in the right IFG was preserved in the TD group, but reduced relative to the quiet condition in ASD groupNon-verbal IQ: TD>ASDNoise: reduced normalized coherence in the beta band (14–25 Hz) between left temporal and left inferior frontal sub-regionsUnnormalized coherence significantly increased in ASD in multiple frequency bandsMatsuzaki et al. (2017)MEGMMFMMF and M100: children with ASD who experience abnormal auditory sensitivityAuditory oddball paradigm (standard 300 Hz, deviant 700 Hz)ASD_S : longer temporal and frontal residual M100/MMF latenciesND: IQ (mean) > 100ASD_SASD_noSTDASD_SASD_noSTDProlonged residual M100/MMF latencies were correlated with the severity of abnormal auditory sensitivity in temporal and frontal areas of both hemispheres119139.62 (1.82)9.07 (1.31)9.45 (1.51)Yoshimura et al. (2017)MEGMMFPresence of a speech onset delay (ASD - SOD and ASD - NoSOD)Oddball standard stimuli (456 times, 83%) and deviant stimuli (90 times, 17%)ASD: decreased activation in the left superior temporal gyrus (MMF amplitude)Mental Processing ScaleASD-SODASD - NoSOD46ASD-SODASD - NoSOD58.4 (37–79)ASD: significant negative correlation between the MMF amplitude in the left pars orbitalis and language performanceASD-SOD < ASD-NoSOD232458.1 (40–72)62.5 (40–72)ASD - SOD: exhibited increased activity in the left frontal cortex (i.e., pars orbitalis)ASD-SOD < TDVocabulary TD>ASDBrennan et al. (2016)MEGReceptive cascading effects on speech sound processingBeamformer source analysis was used to isolate evoked responses (0.1–30 Hz) to stimuli in the left and the right auditory cortexNonce linguistic stimuli that either did or did not conform to the phonological rules that govern consonant sequences in EnglishPhonological processing is impacted in ASDIQ TD > (ASD) > 9012139.3 (1.4)9.7 (1.4)Right auditory attenuated response to illegal sequences relative to legal sequences that emerged around 330 ms after the onset of the critical phonemeGanesan et al. (2016)MEGCortical auditory evoked responsesSomatosensory domain in rapid processing of tactile pulsesSequence of two tactile pulses with different (short and long) temporal separationNo group difference in the evoked response to pulses with long (700 ms) temporal separationND: verbal, and non-verbal IQ > 100122212.5 (5.21)13.77 (3.72)No group differences in the evoked responses to the sequence with a short (200 ms) temporal separationTouch score TD > ASDKurita et al. (2016)MEGAEF synchronizationGlobal coordination across spatially distributed brain regions using Omega complexity analysis - global coordination of AEFsASD: higher Omega complexities time-window 0–50msND: IQ (mean) > 90505066.7 (38 – 92)66.8 (36 – 97)Lower right-left hemispheric synchronizationmmPort el al. (2016)MEGAuditory response maturationLongitudinal bilateral primary/secondary auditory cortex time-domain (100 ms evoked response latency (M100)) and spectrotemporal measures (gamma-band power and inter-trial coherence (ITC))Sinusoidal pure tonesASD_1 + ASD_2: M100 latencies delayed, associated with clinical ASD severityND Full IQ >100ASD"had ASD"9Timepoint 18.4 (1.1)8.7 (0.7)8.4 (1.3)ASD: gamma-band evoked power and ITC reducedVerbal Comprehension TD>ASD225Timepoint 212.1 (1.3)11.8 (0.4)11.9 (1.5)ND: M100 latency and gamma-band maturation rates "had-ASD": exhibited M100 latency and gamma-band activity mean values in-between TD and ASD at both time-pointsYau et al. (2016)MEGSpeech and non-speech processingAssociation between poor spoken language and atypical event-related field (ERF) responsesSpeech and non-speech soundsASD: poor spoken language scores associated with atypical left hemisphere brain responses (200 to 400 ms) to both speech and non-speechIQ TD > (ASD)141810.81 (1.71)10.02 (2.39)Edgar et al. (2015)MEGNeuromagnetic Oscillations phenomenaTest oscillatory phenomena in ASD in terms of frequency and time (STG auditory areas)Pure tones at 200, 300, 500, and 1,000 HzASD: pre-stimulus abnormalities across multiple frequenciesND IQ > 1001053610.07 (2.37)10.90 (2.78)Early high-frequency abnormalities followed by low-frequency abnormalitiesCore language TD > ASDGandhi et al. (2015)GSR, MEGAuditory habituationAutonomic and electrophysiological sensitivity and habituation1st GSR (beep presentation)Consistent patterns of reduced habituation in ASDNo IQ measures obtained131327.1 (5.9)28.9 (5.1)GSR_TD: predicted steady decline consistent with habituationGSR_ASD: no decline + steady increase in the GSR over the course of the session2nd MEG (early vs late responses)MEG_TD: early ERFs stronger15.12 (5.6)14.75 (5.9)MEG_ASD: unchanged amplitude ERFs over timeASD-MVNV* minimally verbal or non-verbal children who have ASD, ASD-V verbal individuals who have ASD and no intellectual disability, IFG inferior frontal gyrus, RTG right temporal gyrus, STG superior temporal gyrus, LI language impairment, AEF auditory evoked field, ERFs sensory evoked response fields, ASSR auditory steady-state response, SF sustained field, SS defined based on the CELF-4 core language index percentile, ASD-SOD presence of a speech onset delay, pSTG posterior superior temporal gyrus, ROIs regions of interest, GSR galvanic skin response, ASD_S with abnormal auditory sensitivity, ASD_noS without abnormal auditory sensitivity, MRS magnetic resonance spectroscopy, Gamma gamma-band activitySurprisal = quantify how much information a particular word contributes given some linguistic context. Unexpected words contribute more information—they have high surprisal—as compared to highly expected words"had-ASD" = subjects with ASD at timepoint 1, and not at timepoint 2Significantly different from TD at p < 0.001; **Significantly different from TD at p < 0.01; Significantly different from TD at p < 0.05Table 11Summary of publications sources using MRI, organized by yearSourceFieldMethodExperimentnMean age (SD)ParadigmTask/stimuliResultsCognitive standard scoresRelevant resultsASDTDor Mean age (min range–max range)ASDTDCharpentier et al. (2020)Brain hemodynamicfMRIOddball paradigmBrain responses to vocal changes with different levels of saliency (deviancy or novelty) and different emotional content (neutral, angry).Brain processing of voice and deviancy/novelty appears typical in adults with ASDND performance IQ141627.9 (6.4)26.4 (7.5)No group difference between control and ASD was reported for vocal stimuli processing or for deviancy/novelty processing, regardless of emotional contentVerbal IQ TD > ASDMurray et al. (2020)Cortical neural inhibitionfMRIDisrupted cortical neural inhibition and neural responsesComparing fMRI response magnitudes to simultaneous visual, auditory, and motor stimulationASD: No increases in the initial transient response in any brain region - there is no increase in overall cortical neural excitabilityND: mean IQ > 10018322324ASD: widespread fMRI magnitude increases in response following stimulation offset, approximately 6–8 s after the termination of sensory and motor stimulationASD: higher fMRI offset - attributed to a lack of an “undershoot”TD: Offset response magnitude associated with reaction times (RT)ASD: overall reduced RTRaatikainen et al. (2020)Whole-brain dynamics3D magnetic resonance encephalographyWhole-brain dynamic lag pattern variationResting-state networks (RSNs)10.8% of the 120 RSN pairs had statistically significant dynamic lag pattern differences that survived correction with surrogate data thresholdingND: mean GAI > 100202023.7 (3.2)25.3 (6.2)Novel technique called dynamic lag analysis (DLA)Alterations in lag salience, executive, visual, and default-mode networks92.3% of the significant RSN pairs : shorter mean and median temporal lags in ASD (84.6% TD)Pegado et al. (2020)Temporal voice areafMRIThe “population thinking”: audio-visual ‘social norm inference’ taskImagine how most people would judge the appropriateness of vocal utterances in relation to different emotional visual contextsASD: more interindividual variability in these judgments despite equal within-participant reliabilityND: mean IQ > 100222222.5 (4.09)22.8 (2.94)Watching a visual display and hearing auditory input (vocal reaction)ASD + TD: similar neural representationsASD: more interindividual variability at TVALarger neural idiosyncrasy in a high-level auditory area - larger behavioral idiosyncrasy (judging auditory valence)Abrams et al. (2019)Voice processingfMRISocial communication abilities and activation in key structures of reward and salience processing regionsNeural responses elicited by unfamiliar voices and mother’s voiceASD: Functional connectivity between voice-selective and reward regions during voice processing predicted social communicationND full-scale IQ > 100212110.75 (1.48)10.32 (1.42)Aggarwal and Gupta (2019)Dynamic functional brain networksfMRIMultivariate graph learningResting-state brain networksASD: dynamic functional brain networks alteredND: mean IQ > 100Dataset 1352611.17 (1.49)10.9 (1.62)ASD: alterations in multiple functional brain networks including cognitive control, subcortical, auditory, visual, bilateral limbic, and default-mode network.Dataset 2398510.49 (1.53)10.44 (1.49)Green et al. (2019)Neural Habituation and GeneralizationfMRISensory over-responsivity and brain response in sensory-limbic regionsThree fundamental stages of sensory arousal (i.e., initial response), habituation (i.e., change in response over time), and generalization of response to novel stimuliHigh_SOR_ASD: Reduced ability to maintain habituation in the amygdala and relevant sensory cortices and to maintain inhibition of irrelevant sensory corticesND full IQHigh_SOR212713.28 (3.35)13.53 (2.79)Low-SOR_ASD: distinct, nontypical neural response patterns, including reduced responsiveness to novel but similar stimuli and increases in prefrontal-amygdala regulation across the sensory exposureVerbal IQ High_SOR < TDLow_SOR2114.22 (2.32)Tietze et al. (2019)Speech perceptionfMRIAudiovisual integration deficits in Aspergr syndromeSemantic categorization disyllabic AV congruent and AV incongruent nounsTD: stronger activation left auditory cortex (BA41)ND: verbal IQ161639.50 (11.17)33.75 (8.22)Watanabe et al. (2019)Neural timescalefMRIIntrinsic neural timescaleResting-state networks (RSNs)ASD + TD: similar whole-brain pattern of intrinsic neural timescalesND2526≥18 years oldLonger timescales in frontal and parietal corticesFull/verbal/performance IQ ≥ 80Shorter timescales in sensorimotor, visual, and auditory areasLloyd-Fox et al. (2018)DevelopmentfNIRSProspective longitudinal study 36 monthsHuman vocalizations compared to non-vocal soundsASD: reduced activation to visual social stimuli across IFG and pSTS-TPJDevelopmental ability TD > ASDHigh-risk ASD2016149.35 days (27.28)153.81 (25.67)First months of life -> later developed ASD 3 years oldReduced activation to vocal sounds and enhanced activation to non-vocal sounds within MTG-STGASD516Millin et al. (2018)AdaptationfMRIAuditory cortical adaptationRepeated audiovisual stimulation in early sensory cortical areasInitial transient responses equivalent ASD and TDND full-scale IQ > 10024292323ASD: in auditory but not visual cortex, greater post-transient sustained response in the fixed-interval timing conditionASD: individual differences in the sustained response in auditory cortex correlated with symptom severityGreen et al. (2018)SORfMRIAversive sensory stimuli and attentional modulationInterpreting communicative with and without a tactile sensory distracter, and with and without instructions directing their attention to relevant social cuesASD: decreased activation in auditory language and frontal regions for task in the presence of the sensory distracter,ND mean full-scale IQ > 100151614.09 (2.70)14.97 (2.44)ASD: increased medial prefrontal activity during tactile stimulationGreen et al. (2017)Thalamocortical connectivity and SORfMRIRole of pulvinar connectivity during mildly aversive sensory inputASD: aberrant modulation of connectivity between pulvinar and cortex (including sensory-motor and prefrontal regions) during sensory stimulationND Mean Full-scale IQ > 100191913.71 (1.60)13.61 (2.57)ASD: pulvinar-amygdala connectivity was correlated with severity of SOR symptomsLinke et al. (2018)ConnectivityfMRIInterhemispheric and thalamocortical functional connectivityNo taskAtypical processing of sounds related to social, cognitive, and communicative impairmentsND: mean IQ > 100403814.02 (2.76)13.66 (2.65)ASD: severity of sensory processing deficits and lower verbal IQ related to reduced inter-hemispheric connectivity of auditory corticesASD: Increased connectivity between the thalamus and auditory cortex - associated with reduced cognitive and behavioral symptomatologyFloris et al. (2016)Structural lateralizationfMRILeft and right-hemisphere specializationStructural asymmetries in cortical regions of interestASD: stronger rightward lateralization within the inferior parietal lobuleND mean full-scale IQ > 100676926.19 (6.79)27.88 (5.99)Measures of language, motor, and visuospatial skillsASD: reduced leftward lateralization extending along the auditory cortex comprising the planum temporale, Heschl’s gyrus, posterior supramarginal gyrus, and parietal operculumPerformance IQ TD > ASD**More pronounced in ASD individuals with delayed languageGreen et al. (2016)Salience Network Connectivity and SORfMRISOR symptoms related to salience network connectivityBrain response to mildly aversive tactile and auditory stimuliASD: SOR related with increased resting-state functional connectivity between salience network nodes and brain regions implicated in primary sensory processing and attentionND mean full-scale IQ > 100283312.95 (1.98)12.93 (2.98)Resting-state salience network connectivityASD: strength of this connectivity at rest is related to extent of brain activity in response to auditory and tactile stimuli.Hoffmann et al. (2016)Social perception networkfMRIActivation and connectivity analysesFace-, voice-, and audiovisual-processing brain regionsASD: reduced connectivity between the left temporal voice area (TVA) and the superior and medial frontal gyrusND102032.22 (9.96)31.11 (11.12)ASD: connectivity between the left TVA and the limbic lobe, anterior cingulate and the medial frontal gyrus as well as between the right TVA and the frontal lobe, anterior cingulate, limbic lobe and the caudate decreased with increasing symptom severitySchelinski et al. (2016)Voice processingfMRIVoice processingVocal sound and voice-identity recognitionASD: dysfunction in voice-sensitive regions during voice identity but not speech recognition in the right posterior superior temporal sulcus/ gyrus (STS/STG)ND mean full-scale IQ > 1001633.75 (10.12)33.69 (9.58)TD: right anterior STS/STG correlated with voice-identity recognition performanceASD + TD: Passive listening to vocal, compared to non-vocal, sounds elicited typical responses in voice-sensitive regionsWatanabe and Rees (2016)Gray matterMRIRelative gray matter volumes (rGMVs)Measure cortical networks, how they changed with age, and their relationship with core symptomatology.ASD: age-associated atypical increases in rGMVs of auditory and visual networksND mean full-scale IQ > 100Children899612.4 (3.0)13.1 (2.6)Public neuroimaging dataASD: age-related aberrant decrease in rGMV of a task-control system (fronto-parietal network, FPN)ND mean full-scale IQ > 100Adults345023.9 (5.5)24.0 (5.0)Enlarged rGMV of the auditory network in ASD adults - associated with the severity of autistic socio-communicational core symptomVisual network—correlated with the severity of restricted and repetitive behaviorsYamada et al. (2016)Insular cortexfMRIResting stateSub-regional organization of the insula and the functional characteristics of each sub-regionASD: alterations in the anterior sector of the left insula and the middle ventral sub-region of the right insulaND mean full-scale IQ > 100363829.9 (7.1)32.5 (7.3)Data-driven clustering analysisTD: anterior sector of the left insula contained two functionally differentiated sub-regions for cognitive, sensorimotor, and emotional/affective functionsASD: single functional cluster for cognitive and sensorimotor functions-anterior sectorASD: volumetric increase right insulaAV* audiovisual integration, MEG magnetoencephalography, MRI magnetic resonance imaging, MRS Magnetic Resonance Spectroscopy, TVA * “Temporal Voice Area”, GAI General Ability Index, IFG inferior frontal, pSTS-TPJ posterior temporal, MTG-STG left lateralised temporal, BOLD Blood Oxygenation Level Dependent, SOR Sensory over-responsivity, Glu Glutamate, Glx glutamine, ND no differencesTable 12Summary of publications sources using several multimodal tools, organized by yearSourceFieldMethodExperimentnMean age (SD)ParadigmTask/stimuliResultsCognitive standard scoresRelevant resultsASDTDOr Mean age (min range- max range)ASDTDPierce et al. (2021)Spontaneous brain activityEEG-MRSResting-state alpha powerMRS [] excitatory (Glu + Glx) and inhibitory (GABA)Decreased resting alpha power > 100313111.3 (1.6)10.6 (1.9)NeurochemicalConcentrations of excitatory and inhibitory neurotransmittersND: GluGlx in the temporal-parietal junctionRoberts et al. (2020)Structural and neurochemical factorsMEGIdentify and contrast the multiple physiological mechanismsSinusoidal tones of 500 Hz frequency (300 ms duration; 10 ms ramps) with a pseudo-randomized 600–2000-ms inter-trial interval were presented at 45-dB sensation level, after individual hearing threshold determinationAuditory radiation fractional predict 52% of M50 latency TDAbove the second percentile (SS > 70) on the non-verbal reasoning composite score of the cognitive assessment774011.4 (2.4)11.5 (2.8)Brain’s response time to auditory tonesMRIAssociated with auditory processing efficiencyAuditory radiation fractional predict 12% of M50 latency ASDGABA MRSASD: altered patterns of M50 latency modulation characterized by both higher variance and deviation from the expected structure–function relationship established with the TD groupTD M50 latency model identified subpopulation of ASD—outliers of TDSubpopulation of ASD: unexpectedly long M50 latencies in conjunction with significantly lower GABA levelsBloy et al. (2019)Lexical accessMEGNeurophysiological marker of language abilityWords and plausible, pronounceable non-wordsIntegral of event-related desynchronization in the 5–20 Hz band during 0.2–1 s post auditory stimulation with interleaved word/non-word tokensND: IQ (mean) > 100 35159.4 (1.1)8.8 (1.4)Structural MRICorrelation with clinical assessment of language function in both ASD and TDLanguage TD > ASD**Not related to general cognitive ability nor autism symptom severityDe Stefano et al. (2019)Oscillatory activity in response to auditory stimuliEEGDrive the cortex to oscillate at a range of frequenciesTone amplitude-modulated by a sinusoid linearly increasing in frequency from 0–100 Hz over 2 sOlder ASD: decreased ability to phase-lock to the stimulus in the low gamma frequency rangeIQ > 90Child778.86 (1.77)8.71 (1.50)ND between young ASD + TDAdult8816.5 (4.14)18.00 (4.90)Developmental different for low gamma-powerTD show decrease gamma-power, while ASD did notLow gamma STP: correlated with increased clinical scores for repetitive behaviorsBorowiak et al. (2018)Visual-speech recognitionfMRIExtracting speech information from face movementsLip reading; PPI analysisASD: decreased BOLD response during visual-speech recognition in the right visual area 5 (V5/MT) and left temporal visual-speech area (TVSA)ND full-scale IQ > 851717Eye trackingASD: right V5/MT—positive correlation with visual-speech taskASD: lower functional connectivity between the left TVSA and the bilateral V5/MT and between the right V5/MT and the left IFGASD and TD = similar responses in other speech-motor regions and their connectivityTanigawa et al. (2018)Language ProcessingMRISurface-based morphometric structure analysisAuditory word comprehension taskNo structural differencesND: mean IQ > 100161713.4 (1.1)13.4 (1.2)MEGCortical responsesASD: correlation between volume of the left ventral central sulcus (vCS) and linguistic scoresASD: weaker cortical activation in the left vCS and superior temporal sulcusASD: atypical gamma-band (25–40 Hz) network centered on the left vCSBerman et al. (2016) Integratation of diffusion MR measures of white-matter microstructure and MEG measures of cortical dynamicsMEG Associations between brain structure and function within auditory and language systems Diffusion MR delineate and quantitatively assess the auditory radiation and arcuate fasciculus segments of the auditory and language systemsASD: Atypical development of white matter and cortical functionNo reference of IQ95 4410.2 (2.6)10.4 (2.4)Diffusion MRIASD: Atypical lateralizationLanguage M100: marker of ASD severity; MMF language impairmentLI: SS < 85TD: SS > 70Port et al. (2016)E/I balance and GammaMEGMEG, MRI and MRS data200, 300, 500, and 1000 Hz (300 ms duration; 10 ms ramps) sinusoidal tonesAuditory cortex localized phase-locked Gamma was compared to resting Superior Temporal Gyrus relative cortical GABA concentrations for both children/adolescents and adultsSS > 70Children271111.7 (0.36)10.6 (0.56)MRIChildren/adolescents_ASD: decreased GABA1/Creatine (Cr) levels, though typical GammaAdults152121.9 (1.1)27.0 (1.2)MRSChildren/adolescents_ASD: lack of typical maturation of GABA1/Cr concentrations and gamma-band coherenceChildren/adolescents_ASD: failed to exhibit the typical GABA1/Cr to gamma-band coherence associationSadeghi Bajestani et al. (2016)Hemispheric asymmetryEEGExtracted two Indexes: Divergence (D) and number of Poincaré section points further from thresholdAnimation with audio (V-A) for 5 min and watching the animation with muted audio band (VwA)Hemispheric asymmetry in ASD children does not follow norm patterns–6060Range: 3–11Range: 3–11Edgar et al. (2015)Maturation of auditory cortical responsesMEGAuditory time-domain and time–frequency activityTones: 500- and 1000-Hz tones of 300-ms duration (binaurally)ASD: right STG M100 latency delayND: IQ (mean) > 100 526310.1 (1.7)9.8 (1.8)MRIT1-weighted structural MRILeft and right STG: greater pre- to post-stimulus increase in 4- to 16-Hz TP for both tones in ASD versus TDC after 150 msLeft and right 50-ms (M50), 100-ms (M100), and 200-ms (M200) time-domain and time–frequency measures (total power (TP) and inter-trial coherence (ITC))Right STG: greater post-stimulus 4- to 16-Hz ITC for both tones was observed in TDC versus ASD after 200 msAge left and right M200 decreasing with age in TDC but significantly less so in ASDAV audiovisual integration, MEG magnetoencephalography, MRI magnetic resonance imaging, MRS Magnetic Resonance Spectroscopy, *TVA * “Temporal Voice Area”, GAI General Ability Index, IFG inferior frontal, pSTS-TPJ posterior temporal, MTG-STG left lateralised temporal, BOLD Blood Oxygenation Level Dependent, SOR Sensory over-responsivity, Glu Glutamate, Glx glutamine, ND no differences
Magnetic resonance imaging (MRI) is an imaging technique that is used to assess the anatomy and physiology of brain circuits. Magnetoencephalography (MEG) is a functional neuroimaging technique that detects, records, and analyzes the magnetic fields produced by electrical currents occurring naturally in the brain (Cohen 1972). While EEG records brain electrical fields, MEG records magnetic fields. Similar to EEG and ERPs, MEG signals can be also time-locked to particular events, being called event-related magnetic fields (ERFs). As previously described for N100 (EEG signal), M100 (MEG) refers to a peak signal occurring at a latency of about 100 ms after stimulus onset. Both MEG and EEG are non-invasive methods for recording neural activity providing data with high temporal resolution (measured in milliseconds), thus providing unique information in terms of timing, synchrony, and connectivity of neural activity (Port et al. 2015). Despite the fact that EEG signals might display superimposed sources of activity, EEG is useful to quickly determine how brain activity can change in response to stimuli and to directly detect abnormal activity, having the advantage of being fully or semi-portable with an accessible cost for researchers. MEG has the advantage that the local variations in conductivity of different brain matter do not attenuate the signal, providing more accurate spatial resolution of neural activity than EEG (Landini et al. 2018). Regarding EEG and MEG use in young children, these two techniques offer advantages over some neuroimaging techniques, including fewer physical constraints and the absence of radiation and noise (Port et al. 2015). Still, EEG and MEG have limited spatial resolution, making it difficult to determine the precise location of neuronal activity with confidence. In contrast, MRI provides data with good spatial resolution, but lacks a good temporal resolution at the electrophysiological level and cannot provide frequency band discrimination. Functional magnetic resonance imaging (fMRI) uses MRI to measure the oxygenation of blood flowing near active neurons, being a valuable tool for delineating the human neural functional architecture (Cole et al. 2010). Combining EEG/MEG with MRI can increase the spatial resolution of electromagnetic source imaging, while tracing the rapid neural processes and information pathways within the brain (Liu et al. 2006), making them good candidates for multimodal integration.
Results from studies with high-functioning ASD individuals show delayed latencies at M50 and M100 auditory evoked responses, suggesting impairments at early auditory processes in the primary and secondary auditory cortex (Claesdotter-Knutsson et al. 2019; Matsuzaki et al. 2020; Roberts et al. 2019; Port et al. 2016; Edgar et al. 2013). It is thought that the major activity underlying M100 is located in the supratemporal plane, with superior temporal gyrus (STG) as the primer M50 generator (Edgar et al. 2015). STG results from the ASD group suggest increased pre-stimulus abnormalities across multiple frequencies with an inability to rapidly return to a resting state before the following stimulus (Edgar et al. 2013). Neurotypical individuals present a negative association between age and latency of M50 and M100 (Matsuzaki et al. 2020; Roberts et al. 2020), which indicates a functional decrease with age. Results show a similar pattern for children with ASD regarding M50, but not with M100 latencies (Matsuzaki et al. 2020). A group of ASD children and TD peers were compared at two time-points, from approximately 8 to 11 years old, showing M100 latency and gamma-band maturation rates similar between both groups (Port et al. 2016). A study of cascading effects on speech sound processing found lower brain synchronization in the early stage of the M100 component for ASD children (Brennan et al. 2016). A group of younger ASD children with approximately 5 years old was assessed in a different study, showing shorter M100 latencies in the left hemisphere (Yoshimura et al. 2021). The M200, considered an endogenous response associated with attention and cognition, seems to have a maximum amplitude around 8 years old, decaying with age. This pattern of age-dependent decrease in neurotypical children was less clear in the ASD group (Edgar et al. 2015), indicating perhaps a maturational delay.
Looking at data across lifespan from individuals with ASD without intellectual disability, delayed latencies were found above 10 years old versus shorter latencies in younger children, suggesting atypical brain maturation in ASD. Minimally verbal or non-verbal children with ASD (ASD-MVNV) seem to present greater latencies delays in M50 and M100 (components associated with language and communication skills) compared to ASD children without intellectual disabilities (Roberts et al. 2019). Similar association for verbal comprehension was found in the left auditory cortex regarding M200 latency response (Matsuzaki et al. 2017; Demopoulos et al. 2017). In auditory vowel-contrast mismatch field experiments (MMF), an association was found between MMF delay and language impairments in children with ASD (Berman et al. 2016). Furthermore, in a study testing pre-attentive discrimination of changes in speech tone, the amplitude of the early MMF component (100–200 ms) seems to be decreased in left temporal auditory areas for ASD children (Yoshimura et al. 2017). This group of ASD children, also diagnosed with speech delay, seem to have increased activity in the left frontal cortex compared to other ASD children without speech delay (Yoshimura et al. 2017). Deficits in auditory discrimination have also been reported in children with ASD, namely bilaterally delayed MMF latencies (Matsuzaki et al. 2019a) as well as rightward lateralization of MMF amplitude (Matsuzaki et al. 2019b) contrasting with the leftward lateralization found in NT children (Matsuzaki et al. 2019a). ASD children with abnormal auditory sensitivity seem to have longer temporal and frontal residual M100/MMF latencies (Matsuzaki et al. 2017). These findings were correlated with the severity of auditory sensitivity in temporal and frontal areas for both hemispheres (Matsuzaki et al. 2017). Taking these data together, ASD seems to be characterized by atypical neural activity in the auditory cortex, together with impaired auditory discrimination in brain areas related to attention and inhibitory processing. Such findings seem to be highly associated with language and comprehension deficits.
EEG and MEG can be transformed to decompose its raw signal into frequency band components. In adults, the typical frequency bands and their approximate spectral boundaries are delta (δ, from 1 to 3 Hz), theta (θ, from 4 to 7 Hz), alpha (α, from 8 to 12 Hz), beta (β, from 13 to 30 Hz), and gamma (γ, from 30 to 100 Hz) (Saby and Marshall 2012). Regarding ASD studies, decreased resting alpha power has been observed in children with ASD (Pierce et al. 2021). In noise experiment conditions, ASD children seem to have increased recruitment of neural resources, with reduced beta band top–down modulation (required to mitigate the impact of noise on auditory processing) (Mamashli et al. 2017). Interestingly, in quiet conditions, no differences were found between ASD and TD peers (Mamashli et al. 2017). A different study using sensory distracters (distracters that disrupts the processing of social cue interpretation) found decreased activation in auditory language and frontal regions in high-functioning youth with ASD (Green et al. 2018).
In auditory habituation studies measuring galvanic skin response, an aversion effect has been reported in ASD, likely due to sensory information overload. Results show consistent patterns of reduced habituation in ASD individuals, without the predicted steady decline that would be expected for habituation experiments. Instead, ASD adults showed a steady increase in the galvanic skin response over the course of the sessions (Gandhi et al. 2021). Regarding phase-lock auditory stimuli, no differences were found in the low gamma frequency range between ASD and TD children around 8 years old. A decrease in low gamma-power was observed in TD subjects around 17 years old but not in the ASD group (Stefano et al. 2019). The atypical gamma-band network in ASD seems to be located around the left ventral central sulcus (vCS) in children around 10 years old (Floris et al. 2016). Older ASD participants showed more pronounced low gamma deficits (Stefano et al. 2019), suggesting an increased background gamma-power that, similar to noise, can affect proper processing of stimuli. Interestingly, a recent study tested ASD children with and without atypical audiovisual behavior and found that only children with atypical audiovisual behavior showed increased theta to low gamma oscillatory power in the bilateral superior temporal sulcus and temporal region (Matsuzaki et al. 2022).
Proper development of the central nervous system requires a fine balance between excitatory and inhibitory (E/I) neurotransmission. This E/I balance seems to be very important for cortical gamma-band activity, given that gamma waves are generated through connections between GABAergic inhibitory interneurons and excitatory pyramidal cells (Stefano et al. 2019; Port et al. 2017). A multimodal imaging study combined MEG, MRI, and GABA magnetic resonance spectroscopy (MRS) to assess physiological mechanisms associated with auditory processing efficiency in high-functioning children/adolescents with ASD. The study found longer M50 latency combined with decreased GABA in the left hemisphere for ASD individuals, suggesting an association between sensory response latency and synaptic activity (Roberts et al. 2020). Similar results were shown in a multimodal study that assessed cortical GABA concentrations and gamma-band coherence in the auditory cortex and superior temporal gyrus. Decreased GABA1/Creatine levels were found in children/adolescents with ASD, without the gamma-band coherence association typically seen in neurotypical subjects (Port et al. 2017). A different study combining EEG and MRS showed reduced glutamine in the temporal–parietal cortex associated with greater hypersensibility to sensory input detection (Pierce et al. 2021). A post-mortem study assessed the cytoarchitecture of the anterior superior temporal area (area of Brodmann), involved in auditory processing and social cognition, by quantifying the number and soma volume of pyramidal neurons in the supragranular and infragranular layers (Kim et al. 2015). Results showed no differences between ASD adolescents and adults age-matched with a neurotypical group (Kim et al. 2015). A different study looked at cortical neural inhibition for auditory, visual, and motor stimulation (Murray et al. 2020). Results showed no increase in the initial transient response in ASD individuals, with widespread changes in stimulus offset responses (Murray et al. 2020). Although results show similar patterns of transient response in ASD and TD groups for all cortical regions, larger fMRI amplitudes were found at later response components, approximately 6–8 s after stimulus presentation (stimulus duration of 20 s) (Murray et al. 2020). These studies suggest cortical excitatory–inhibitory imbalance in areas related to auditory processing in subjects with ASD.
Sensory sensitivities can be assessed at three different stages of sensory initial response to the stimuli, habituation, and generalization of response to novel stimuli. Brain imaging studies in individuals with ASD have found auditory discrimination deficits (Matsuzaki et al. 2019a; Abrams et al. 2019), as well as increased neural responsiveness upon repeated stimuli, with larger fMRI response in the auditory cortex that seems specific to temporal patterns of stimulation (Millin et al. 2018). Children with high sensory over-responsivity showed reduced ability to maintain habituation in the amygdala (Green et al. 2019), together with increased resting-state functional connectivity between salience network nodes and brain regions implicated in primary sensory processing and attention (Green et al. 2018). Children with low sensory over-responsivity showed atypical neural response patterns, with increased prefrontal–amygdala regulation across sensory exposure (Green et al. 2019). A different study found intact temporal prediction responses with altered neural entrainment and anticipatory processes in children with ASD (Beker et al. 2021). These results might explain atypical behavioral responses observed in ASD during sensory processing, mediated by top–down regulatory mechanisms.
Differences in response to sound familiarity have also been reported in children with ASD, with reduced activity in right-hemisphere planum polare for unfamiliar voices, reduced activity in a broad extent of fusiform gyrus bilaterally, and less activity in the right-hemisphere posterior hippocampus (Abrams et al. 2019). In a different fMRI study, the authors compared brain responses to vocal changes with different levels of stimulus saliency (deviancy or novelty) and different emotional content (neutral, angry) (Charpentier et al. 2020). Results show no differences between ASD and neurotypical adults regarding vocal stimuli and novelty processing, independently of emotional content. Brain processing appears typical in both groups, with activation in the superior temporal gyrus, and with larger activation for emotional compared to neutral prosody in the right hemisphere (Charpentier et al. 2020). These results suggest that the processing of emotional cues may be placed at later processing stages, such as insular activation, or at the hippocampus level. Interestingly, a recent study show altered voice processing in ASD which seems to be present already at the midbrain level of the auditory pathway (Schelinski et al. 2022).
Deficits in auditory discrimination have also been found both in MEG and brain imaging studies (Ganesan et al. 2016; Claesdotter-Knutsson et al. 2019; Abrams et al. 2019). Individuals diagnosed with ASD seem to have deficits in predicting the offset of standard tones, engaging less resources for duration tasks compared with pitch discrimination tasks (Lambrechts et al. 2018). Spectrally complex sounds can trigger two continuous neural MEG responses in the auditory the auditory steady-state response (ASSR) at the frequency of stimulation, and the sustained deflection of the magnetic field (sustained field).
The ASSR is an oscillatory response phased-locked to the onset of the stimulus, where the frequency of stimulation is represented by the same frequency in the primary auditory cortex (Stroganova et al. 2020). Both ASD and neurotypical children with 5–6 years old seem to show right dominant 40 Hz ASSR (Ono et al. 2020). No differences were found regarding neural synchrony at 20 Hz for both ASD and TD children between 5 and 12 years old (Stroganova et al. 2020; Ono et al. 2020), suggesting a normal maturation of ASSR for low frequencies. Interestingly, the right-side 40 Hz ASSR increased with age in the neurotypical group, as opposed to ASD children (Ono et al. 2020). Reduced 40 Hz power was also found in adolescents with ASD at both right and left primary auditory cortex, with no difference in gamma-band responses (Seymour et al. 2021). Diminished auditory gamma-band responses were found in ASD children, indicating that peak frequencies likely vary with developmental age (Roberts et al. 2021).
The sustained field (SF) is a baseline shift in the electrical and magnetic signals upon exposure to a sound lasting for several seconds. The SF adapts to the probability of a sound pattern, reflecting the integration of pitch information across frequencies within the tonotopic map of the primary auditory cortex (A1) (Stroganova et al. 2020). Children diagnosed with ASD seem to have atypical higher order processing in the left hemisphere of the auditory cortex, with cortical sources of SF located in the left and right Heschl’s gyri (primary auditory cortex) (Stroganova et al. 2020).
The severity of sensory processing deficits in ASD also seems to be correlated with reduced inter-hemispheric connectivity of auditory cortices (Linke et al. 2018; Tanigawa et al. 2018) and lower verbal IQ (Linke et al. 2018). Interestingly, increased connectivity between the thalamus and the auditory cortex was found in patients with reduced cognitive and behavioral symptomatology (Linke et al. 2018; Tanigawa et al. 2018), which suggests high thalamocortical connectivity as a potential compensatory mechanism in ASD (Linke et al. 2018). Individuals diagnosed with ASD also seem to present abnormal modulation of connectivity between pulvinar and cortex, with greater increases in pulvinar connectivity with the amygdala (Green et al. 2017). Regarding processing of social stimuli, reduced connectivity between the left temporal voice area and the superior and medial frontal gyrus was found in ASD patients (Hoffmann et al. 2016). Decreased connectivity between the left TVA and the limbic lobe, anterior cingulate and the medial frontal gyrus as well as between the right TVA and the frontal lobe, anterior cingulate, limbic lobe and the caudate seems to be associated with increased symptom severity (Hoffmann et al. 2016).
Language acquisition involves the integration of top–down and bottom–up processes. Language deficits present in ASD diagnostic criteria may be related to one of these integration processes or a combination of both. ASD individuals can have sensory deficits in the bottom–up early sensory processing and/or prediction deficits related to higher order assessment.
Phonological processing seems to be disrupted in ASD children, displaying attenuated MEG response in the right auditory cortex to both legal and illegal phonotactic sequences (Brennan et al. 2016). Interestingly, ASD children do not seem to have differences in phonological competence but significantly differ in other measures, such as attention, syntax, and pragmatics (Brennan et al. 2016; Wagley et al. 2020), suggesting impairments at language structure knowledge. An event-related desynchrony of the auditory cortex in the 5–20 Hz range seems to index language ability in both children with ASD and neurotypical controls (Bloy et al. 2019). When speech and non-speech were compared, ASD children with poorer language composite scores presented a general auditory processing deficit, with atypical left hemisphere responses in the high order time-window of 200–400 ms (Yau et al. 2016), and different neural and behavioral effects of syllable-to-syllable processing in speech segmentation (Wagley et al. 2020).
When considering visual-speech recognition tasks, ASD individuals seem to have difficulties in extracting speech information from face movements (Borowiak et al. 2018). Decreased Blood Oxygenation Level Dependent (BOLD) responses were detected in the right visual area 5 and left temporal visual-speech area, as well as lower functional connectivity between these two brain regions implicated in visual-speech perception (Borowiak et al. 2018). This multimodal fMRI study combined with eye-tracking data showed that the ASD group had reduced responses not only for emotional but also neutral facial movements (Borowiak et al. 2018). High-functioning adults with ASD seem to have typical responses for voice-identity tasks, and dysfunctional speech recognition in the right posterior temporal sulcus (Schelinski et al. 2016).
Predictive processing was tested in a naturistic environment, by measuring surprisal values, or how much information of word contributes given some linguist context (Brennan et al. 2019). Results showed bilateral temporal effect for sentence-context linguistic predictions in an early time-window (from 26 to 254 ms), for both high-functioning ASD children and TD peers with 3–6 years old (Brennan et al. 2019). A different study showed that as surprisal values increase, the amplitude of the neural response also increases in the left primary auditory cortex, posterior superior temporal gyrus (pSTG), and inferior frontal gyrus (IFG) in neurotypical children (Wagley et al. 2020). However, ASD children with lower IQ levels did not display such learning pattern (Wagley et al. 2020).
A longitudinal study tested children in the first months of life (around 4 months old) who later developed ASD, at 3 years old (Lloyd-Fox et al. 2018). Using functional near-infrared spectroscopy (fNIRS), infants later diagnosed with ASD showed reduced activation to visual social stimuli across the inferior frontal (IFG) and posterior temporal (pSTS-TPJ) regions of the cortex, reduced activation to vocal sounds, and enhanced activation to non-vocal sounds within left lateralized temporal regions (Lloyd-Fox et al. 2018). These results suggest that atypical ASD cortical responses may be detectable at early stages.
The inferior frontal and superior temporal areas in the left hemisphere are crucial for human language processing (Yoshimura et al. 2017). Some striking findings report ASD group differences in left and right hemispheres (Edgar et al. 2013; Sadeghi Bajestani et al. 2017). Results show lower right–left hemispheric synchronization in young children with ASD (Brennan et al. 2016), stronger rightward lateralization within the inferior parietal lobule, and reduced leftward lateralization extending the auditory cortex (Floris et al. 2016). Neurotypical peers show stronger activation in the left auditory cortex for semantic categorization tasks (Tietze et al. 2019), and hemispheric advantage that seems to be absent in ASD children (Edgar et al. 2015). Adolescents diagnosed with ASD show weaker cortical activation in the left ventral central sulcus at word comprehension tasks (Tanigawa et al. 2018), indicating atypical hemispheric functional asymmetries.
Resting-state connectivity is a correlated signal between functionally related brain regions in the absence of any stimulus (spontaneous signal fluctuation). Results show dynamic functional brain networks altered in children diagnosed with ASD, including cognitive control, subcortical, auditory, visual, bilateral limbic, and default-mode network (Stickel et al. 2019). High-functional ASD adults also present alterations in the anterior sector of the left insula and the middle ventral sub-region of the right insula in the ASD brain (Yamada et al. 2016). Atypical spread of activity seems to be present in ASD individuals, indicated by altered dynamic lag patterns in salience, executive, visual, and default-mode networks (Raatikainen et al. 2020). Regarding intrinsic neural timescales, both high-functional adults with ASD and TD peers presented longer timescales in frontal and parietal cortices and shorter timescales in sensorimotor, visual, and auditory areas (Watanabe et al. 2019). Individuals with ASD also seem to display a volumetric increase in the right insula (Yamada et al. 2016). Given that the right insula is primarily specialized for sensory and auditory-related functions, such volumetric expansion might be functionally correlated with previously reported ASD alterations in auditory stimuli processing and auditory sensitivity.
A recent study in children with ASD reports decreased gray matter volume at the fronto-parietal network, associated with the severity of communication score and restricted behaviors. In adults, an increase of gray matter was reported at the regions of auditory and visual networks, with the auditory network being correlated with the severity of the communication core, and visual networks with severity of repetitive and restricted behavior (Yamada et al. 2016). Uncoupled structure–function relationships in both auditory and language networks have also been reported in ASD (Berman et al. 2016), with changes in the relative weight of white matter contribution to structure–function relationships (Roberts et al. 2020).
Despite a large number of studies assessing autism spectrum disorder at the level of auditory processing, it is still not possible to conclude the cause of auditory symptomatology present in ASD. Children and adults diagnosed with ASD have a neurodivergent cognitive profile, and the heterogeneity of both severity and type of symptoms, probably contributes for this lack of causal explanation. Another heterogeneity factor comes from the inclusion criteria for ASD participants, such as the diagnostic assessment confirmation tools or the measurements of IQ levels. Some studies analyze their data considering verbal and non-verbal abilities for ASD children, while other studies refer only to the full performance of IQ levels. To better illustrate this issue, especially for language components assessment, we can look at the study performed by Bloy et al. (2019) that found no differences in IQ mean values between ASD and TD peers, but highly significant differences in language ability. Future studies should include a wider range of standardized assessment tools to determine discrepancies in autistic traits, and larger sample size to avoid limitations in the assessment of within-group and multiple comparisons.
A consideration should also be made about the accuracy of diagnosis of children with ASD. In a longitudinal study, Port and colleagues referred to the inclusion of a group of children with approximately 8 years old considered to be initially on the spectrum. A later follow-up revealed that these children exhibited optimal outcomes at approximately 12 years old, no longer meeting diagnostic criteria for ASD (Port et al. 2016). Interestingly, these children showed results in-between ASD and TD peers. A similar in-between result was found in ASD siblings emotional perceptions (Waddington et al. 2018), indicating a possibility of contextual interference in ASD traits, such as parenting. Sometimes, parents’ perception questionnaires are assessed without taking into consideration the social, economic, and affective influence of parenting and/or children’s educators and peers. When designing auditory research studies, it would be important to also consider other relevant daily-life features, such as special talents, levels of anxiety and aggression, and sensory challenges.
One main limitation of brain imaging and EEG auditory studies in ASD is individual discomfort thresholds, such as sensibility to sound levels or immobility requirements during imaging sessions. By analyzing experimental designs, it is possible to see the wide variety of methods and protocols that are applied, even for similar techniques. For instance, some participants are allowed to sleep during ABR recordings (Fujihira et al. 2021), while some participants watch videos during the experiment (Jones et al. 2020; Chen et al. 2019), creating different conditions to assess similar variables across studies. Another important consideration is medication status as an eligibility criterion for ASD studies. Some studies detail the presence or absence of medication, such as risperidone, anxiolytics, or antidepressants (Port et al. 2016), or simply exclude ASD-medicated participants, while other do not report any criteria regarding medication.
The underlying conceptualization of autism and associated deficits and impairments through the lens of the DSM might push researchers and clinicians to prioritize the correction of perceived deficits as the major goal of behavioral intervention (American Psychiatric Association (APA) 2013; Schuck et al. 2022). Given the neurodiversity and individual differences present in ASD subjects, future studies should ensure a comprehensive neuropsychological evaluation, for both ASD and control subjects. As an example, studies often include the term “high or low functioning”, which is not an official medical diagnosis; hence, it is not clear at every study whether this descriptor is based on full-scale IQ and language, verbal and non-verbal, or adaptive behavior and daily functioning measures. To acknowledge cultural differences, future studies could also include social and ecological validity measures (Schuck et al. 2022), with assessment of the socio-cultural context at individual, institutional, and family levels, using self-report measures. For a better understanding of the human neurocognitive spectrum, both ASD and control subjects should be assessed at other areas of interest, such as self-determination, self-esteem, social inclusion, well-being, personal development, interpersonal relationships, measures of quality of life, and functional adaptive skills (Schuck et al. 2022).
Low-level auditory stimuli (e.g., pitch discrimination) deficits vary widely within ASD, with some interesting differences when low- and high-functioning children (based on IQ assessment) are compared (Table 13). ASD individuals seem better at detecting additional unexpected and expected sounds at several acoustic parameters, showing an increased auditory perceptual capacity, but display deficits in detection and discriminatory tasks, especially in the presence of noise. Difficulties in the processing of sensory stimuli have been confirmed by electrophysiology and brain imaging data at early stages of perceptual processing. ASD patients with verbal disabilities seem to be particularly impaired in terms of cortical processing of acoustic inputs. Larger idiosyncrasy seems to be present in high-level auditory areas, with deficits being associated with severity of social and communication symptoms. One possibility is to look at the core aspects of autism as a cascading effect of unusual auditory and language trajectories (prosody, semantic context). Individuals with ASD seem to have alterations in multisensory integration, displaying poorer performance in multisensory tasks requiring the auditory modality. It is still not clear whether ASD sensory idiosyncrasy affects all types of audiovisual integration and whether these deficits can be compensated by later attentional processes. For non-multimodal studies, further auditory investigation should guarantee that unisensory conditions can be assessed without visual influence (blind conditions) and should control whether auditory processing responses are affected by attention deficits.Table 13Integrity of cognitive functionMain resultsAttentionDeficits in divided, sustained, selective, and spatial attentionND when types of attention are comparedHIGH-FUNCTIONINGAttenuated P3a mean voltagesADULTS: ND P3a latenciesADULTS: Early ERP responses (P50 amplitude) positively correlated to increased sensory sensitivityMSIDistinctive in ASDLOW-FUNCTIONINGHIGH-FUNCTIONINGImpairments at sensitivity to asynchronies (video-audio)Low-level perceptual processesCorrelated with language abilitiesIntact low-level audiovisual integrationGreater multisensory reaction time facilitation for TD adultsHigh-level perceptual processesPoorer multisensory temporal acuityPoorest performances in auditory modality compared to visual modalityAcoustic parameters****HIGH-FUNCTIONINGDeficits in the intensity or loudness of stimuliDeficits in discrimination (e.g., higher auditory duration discrimination threshold of stimuli)Enhanced memory for vocal melodiesEnhanced pitch discrimination–Discrimination ability varies widely within ASDNoiseDetrimental effect of noise and increased arousalWorse speech comprehension in noise conditionND: without noise conditionTemporal processing silent gapsReduced P2 amplitudeSensory habituationLOW-FUNCTIONINGHIGH-FUNCTIONINGReduced habituation P1No reduction between the first and the last ERPDecrease in the amplitude MMNTD: negative slope; SD: positive slopeEnvironmental change****LOW-FUNCTIONINGGreater P3a amplitude to novel soundsYouth: slower attenuation of the N1 response to infrequent tones and P3a response to novel soundsHemisphere activationLOW-FUNCTIONINGHIGH-FUNCTIONINGSpeech detection left hemisphereBilateral attenuationNegative MMN response right hemisphere more activatedError prediction****HIGH-FUNCTIONINGASD + TD: decreased MMNND between ASD + TDN1: similar for ASD and TDMMN modulated by global smaller effect in ASDNo differences P3bReduced superior frontal cortex (FC) to unexpected eventsIncreased dorsolateral prefrontal cortex (PFC) activation to expected eventsLANGUAGEProsodyLOW-FUNCTIONING****HIGH-FUNCTIONINGReduced P1 amplitudediminished amplitude of P3aLarger P3a amplitude (P3a latencies shorter in adults)slower perceptual discriminationEarlier MMNVowel + tonePure-tone: diminished response amplitudes and delayed latency MMN; ND P3aVowel: smaller P3a; ND MMNSpeech vs. non-speechLOW-FUNCTIONINGHIGH-FUNCTIONINGSpeech stimuliNo P1 enhancement as TDN330 match/mismatch responses right hemisphereNonspeech stimuliSimilar P1 enhancementTD: larger MMN responses (speech pitch contour) and stronger MMN (speech pitch height)Nonvocal soundsSmaller P100Smaller right fronto-temporal negative Tb peak non-vocal soundsASD: more positive MMR (speech pitch height)Atypical response to non-vocal soundsSemantic congruence****LOW-FUNCTIONINGN400 effect with shorter latency in TDDelayed speed of processingSONLOW-FUNCTIONINGHIGH-FUNCTIONINGN100 amplitude, SON negativityAuditory filtering disruptionStrength of LPPs positively correlated with auditory filtering abilitiesTDs and ASD-Vs: significant MMRs to OON multisettingNote: descriptor of functioning (low versus high) based on IQ measurements
Difficulties in understanding others are a core feature of autism spectrum disorders (Baron-Cohen 2001). At the emotional level, individuals with ASD seem to have deficits judging auditory valence and vocal emotion recognition, but with normal pro-social functioning, suggesting a normal social awareness and motivation. Future auditory studies should also look into Theory of Mind manifestations, emphasizing social motivation and reward associated with communication. A detrimental effect on communication and increased arousal on ASD children is observed in experiments within a noise context. Interestingly, when the context changes to silent, no differences in speech comprehension are found, suggesting a relevant role of auditory sensory overload in ASD individuals.
Results assessing phonological processing, language components, speech non-speech, and visual-speech recognition, suggest that processing at the auditory cortex is altered in ASD. This atypical sensory processing may interfere with perceptual mechanisms where individuals anticipate what will happen, based on their perceived sensory information. Observed differences in auditory perception in ASD might not be related with attention allocation to acoustic stimuli, but rather to difficulties in recognition and integration of acoustic information, such as the process of understanding speech from other people. Deficits at the level of communicative function would reduce the ability of individuals with ASD to learn several language components, such as phonology, syntax, and semantics. Children use prior information to incrementally narrow down the set of possible interpretations for a sentence, highlight how high-level representations can propagate to low-level processing stages. Deficits in habituation or adaption could potentially lead to an inability to form predictions. Such changes in higher order processing may impact the development of language and interfere with communication.
Integrity of the central nervous system seems to be affected in ASD individuals, with auditory alterations being detectable during early development (Table 14). Several studies indicate atypical brain maturation, abnormal neural network synchronization, and functional alterations in the primary auditory cortex, trailed by impaired cognitive function, such as attention, inhibitory processing, and neural discrimination processes. Most individuals diagnosed with ASD have auditory sensory issues, being mainly hypersensitive to sounds. Some reports also indicate that individuals with ASD may have deficits in lateralized cognitive functions as well as functional and brain structural asymmetry, with disproportionate overgrowth of audio and visual sensory networks. In social tasks involving auditory processing of verbal cues, a reduced connectivity between the left temporal voice area and the superior and medial frontal gyrus has been reported. Interestingly, thalamocortical overconnectivity has been reported in several studies albeit with different it might reflect lack of thalamocortical inhibition (which could cause difficulties in attentional sensory information), or it might be a compensatory mechanism (that could serve to mitigate reduced synchronization).Table 14Integrity of central nervous systemFieldMajor results and conclusionsEvoked-magnetic fields50 and 100High-functioning ASDImpairments at early auditory processesDelayed M50 and M100 latencies children and adults (> 10 years)Short P100 young children (~ 5 years)200Atypical brain maturationM200 lower decrease with ageLeft temporal auditory areasMMF delayLanguageSound discriminationASD: BilateralIndependent of cognitive performanceTD: leftward lateralization of MMF amplitudeImpaired neural discriminationASD: rightward lateralization MMF amplitudeInhibitory processingNoise/distractorAbnormal auditory sensitivityQuiet common neural sourcesNoise MMF response in the right IFG was preserved in the TD group, but reduced relative to the quiet condition in ASD groupNoise: reduced normalized coherence in the beta band (14–25 Hz) between left temporal and left inferior frontal sub-regionsFrequency bands****α decreased resting alpha powerβ reduction in top–down modulationsγ ND youngOlder ASD: deficits low gamma → E/I imbalance → critical periodE/I balanceReduced glutamine in the temporal-parietal cortexDecrease GABA in the left hemisphereNumber and soma volume of pyramidal neuronsInhibition ND early responseIncreases in cortical neural excitability after stimulus offsetAttentionInability to extract the temporal regularities of the stimulation sequenceNeural responsivenessLarger fMRI response in the auditory cortexReduced ability to maintain habituation in the amygdalaIncreased resting-state functional connectivity between salience network nodes and brain regions implicated in primary sensory processing and attentionVoiceEmotional vs. neutral changeTypical brain processingUnfamiliar voicesReduced activity in right-hemisphere planum polareArea of auditory association cortex within the superior temporal gyrusMother’s voiceFusiform gyrusLeft-hemisphere occipital regionsTemporal occipital regions in the right-hemispherePitch processingAtypical processing at the level of the core auditory cortex of the left hemisphereSFLeft and right Heschl’s gyri, anterolateral to ASSRASSRLow consistency of phase dynamics in A1 over timeND 20 HzBrain responses locally dysregulatedReduced 40 Hz ASD (γ)Language****Phonological processingImpaired (attention, syntax and pragmatics)Stronger rightward lateralizationInferior parietal lobuleReduced leftward lateralizationAuditory cortexSpeech and non-speechGeneral auditory processing deficitPlanum temporale, Heschl’s gyrus, posterior supramarginal gyrus, and parietal operculumAtypical left hemisphere responses (200-400 ms)Weaker cortical activation in the left ventral central sulcusSpeech recognitionDysfunction in the right posterior temporal sulcusWeaker activation in the left auditory cortex for semantic categorization tasksVisual-speech recognitionDifficulties in extracting speech information from face↓ BOLD right visual area 5 (V5/MT)Emotional and neutral facial movement both impaired↓ BOLD left temporal visual-speech area (TVSA)ND process of attention allocation (similar eye movement patterns)Predictive mechanismsHigh_functioning: NDLow_functioning: different pattern of TDLexical stressHigh-functioning ASD right hemisphere is more activated than the left hemisphereResting stateChildren: altered dynamic functional brain networksAdults: alterations in the functional organization of the left and right insular sub-regionsVolumetric increase in the right insulaDiffusion****Gray matterIncrease volume with age at auditory cortexDecrease volume task-control systemWhite matterUncoupled structure–function relationships in both auditory and language systemsConnectivityInterhemispheric connectivity increased between the thalamus and auditory cortexThalamocortical overconnectivitySocial reduced connectivity between left temporal voice area and the superior and medial frontal gyrusND no differences between ASD and TD peer
Clinical biomarkers can offer the opportunity to improve predictions, diagnosis, stratification by severity and subtypes, and response indices for pharmaceutical development. Such biomarkers should ideally be robust, sensitive, specific to the disorder, and scale with severity (Port et al. 2015), but finding biomarkers for ASD requires a deep understanding of its neurobiological underpinnings. A correlation between neuroanatomical, genetic, biochemical, and immune findings with clinical ASD diagnosis is still unclear (Levin and Nelson 2015). Furthermore, the heterogeneity of age-related phenotypes in ASD poses a challenge in the pursuit of clinical biomarkers. In that sense, functional signatures derived from electrophysiological and imaging studies might become promising biomarkers given that they offer a temporal layer that could help revealing putative biological trajectories along the development process.
The brain is remarkably malleable, capable of restructuring itself in response to experience. Major sculpting of brain circuits occurs during specific time windows known as critical periods (Leblanc and Fagiolini 2011). Distinct critical periods underlie different modalities, ranging from visual processing to language and social development. Critical periods begin in primary sensory areas and occur sequentially in the brain, requiring a precise balance of excitatory/inhibitory (E/I) neurotransmission (Bourgeron 2009). These periods close after structural consolidation, diminishing future plasticity as the brain reaches adulthood. Although critical periods provide an exceptional time-window for learning and consolidation, they also represent a period of great vulnerability for the developing brain.
Different neurodevelopmental trajectories and brain maturation processes may explain the heterogeneity of behavioral and cognitive traits observed in ASD. Checking the integrity of the peripheral auditory system as a longitudinal measure of auditory maturation seems to hold some predictive value. ABR studies (both click-ABR and speech-ABR) tend to show longer latencies in children with ASD, and several EEG studies show unstable neural tracking in subcortical auditory processing. However, not all children have the same clinical presentation, suggesting the potential existence of auditory processing-related subtypes of children with ASD. Considering the results from ABR studies, one interesting finding is ABR longitudinal profile across development that seems to indicate shorter latencies in newborns, longer latencies in ASD children compared to newborns, no differences in adolescents, and normal ABR in adults. Infants and toddlers later diagnosed with ASD present delayed auditory brainstem responses, mainly with later wave V latencies (Tecoulesco et al. 2020; Ramezani et al. 2019; Chen et al. 2019), that does not seem to persist through development. These findings highlight a potential difference in terms of auditory brainstem maturation timing, or the existence of compensatory mechanisms such as increasing myelin density. Given that ABR testing is relatively non-invasive and low cost, it could be advantageous to study longitudinal auditory brainstem maturation in children at a higher risk for ASD.
Interestingly, diffusion MRI and MEG studies suggest a deficiency in audiovisual temporal processing, with prolonged cortical response in older children with ASD, mainly mismatch negativity and middle latency delays (M50/M100) (Stevenson et al. 2017, 2018), together with atypical development of white matter and cortical function (Berman et al. 2016). Such results could reflect an abnormal maturation of the brainstem that could affect the temporal synchrony of neuronal firing, or/and white matter alterations that could lead to poor signal conduction. Given the range of ASD presentations along development, it could be useful to assess the longitudinal profile of ASD children in a multimodal analysis, comparing the neuropsychological profile, the auditory brainstem maturation, together with an assessment of myelin and cortical response profiles.
The usefulness of longitudinal EEG as a diagnostic tool for uncovering developmental trajectories in ASD has been recently suggested, showing that delta and gamma frequency power trajectories can differentiate autism outcomes, in the first postnatal year (Gabard-Durnam et al. 2019). Furthermore, EEG spectral power has been suggested as a marker to differentiate between low- and high-risk ASD infants at 6 months of age (Tierney et al. 2012), as well as a marker of disease severity in girls with Rett syndrome (Roche et al. 2019). The observation of increased power in the delta band could represent abnormal cortical inhibition due to dysfunctional GABAergic signaling (Roche et al. 2019). Given that auditory-related gamma and alpha powers also seem to be altered in ASD subjects along development (Port et al. 2016; Pierce et al. 2021; Stefano et al. 2019), it would be interesting to assess these measures together with social, cognitive, and language abilities, as potential predictors of later outcomes in ASD.
Not many studies have looked into E/I balance related to auditory processing in ASD. The imbalance hypothesis is highly promising, given the suggestion of cortical excitatory–inhibitory imbalance in areas related to auditory processing in subjects with ASD (Murray et al. 2020). It is also highly promising, since it provides the basis for a number of ASD biomarkers at various levels, from molecules to the neural networks that ultimately determine behavior (Levin and Nelson 2015). For instance, positron emission tomography (PET) is a molecular imaging technique that can be utilized in vivo for dynamic and quantitative measurement of neurotransmitter release in the human brain. Given the clear evidence stemming from animal studies (Castro and Monteiro 2022) showing auditory dysfunction and E/I imbalance in different animal models of ASD, it would be interesting to see results from PET studies looking at excitatory and inhibitory neurotransmitter systems, cerebral glucose metabolism, blood flow perfusion, and inflammation in the CNS in ASD patients, while performing specific auditory tasks for assessment of sensory function. In summary, a multivariate combination of biomarkers may be the most promising tool for a better understanding of the significant role of neurodevelopmental change in ASD.