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Neuroanatomy of Individual Differences in Language in Adult Males with Autism.


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Type

Article

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Authors

Lai, Meng-Chuan 
Lombardo, Michael V 
Ecker, Christine 
Chakrabarti, Bhismadev 

Abstract

One potential source of heterogeneity within autism spectrum conditions (ASC) is language development and ability. In 80 high-functioning male adults with ASC, we tested if variations in developmental and current structural language are associated with current neuroanatomy. Groups with and without language delay differed behaviorally in early social reciprocity, current language, but not current autistic features. Language delay was associated with larger total gray matter (GM) volume, smaller relative volume at bilateral insula, ventral basal ganglia, and right superior, middle, and polar temporal structures, and larger relative volume at pons and medulla oblongata in adulthood. Despite this heterogeneity, those with and without language delay showed significant commonality in morphometric features when contrasted with matched neurotypical individuals (n = 57). In ASC, better current language was associated with increased GM volume in bilateral temporal pole, superior temporal regions, dorsolateral fronto-parietal and cerebellar structures, and increased white matter volume in distributed frontal and insular regions. Furthermore, current language-neuroanatomy correlation patterns were similar across subgroups with or without language delay. High-functioning adult males with ASC show neuroanatomical variations associated with both developmental and current language characteristics. This underscores the importance of including both developmental and current language as specifiers for ASC, to help clarify heterogeneity.

Description

Keywords

autism, individual differences, language, neuroanatomy, specifiers, Adolescent, Adult, Autism Spectrum Disorder, Brain, Humans, Individuality, Language Development Disorders, Magnetic Resonance Imaging, Male, Young Adult

Journal Title

Cereb Cortex

Conference Name

Journal ISSN

1047-3211
1460-2199

Volume Title

25

Publisher

Oxford University Press (OUP)
Sponsorship
Medical Research Council (G0001354)
Medical Research Council (G0600977)
Medical Research Council (G1000183)
This work was supported by the Waterloo Foundation [grant number 921/1247 to S.B-C. and M-C.L.], the UK Medical Research Council [grant number GO 400061 to D.G.M.M., S.B-C. and E.T.B.], and the European Autism Interventions - A Multicentre Study for Developing New Medications (EU-AIMS); EU-AIMS receives support from the Innovative Medicines Initiative Joint Undertaking under grant agreement n° 115300, resources of which are composed of financial contribution from the European Union's Seventh Framework Programme (FP7/2007-2013), from the EFPIA companies in kind contribution and from Autism Speaks. During the period of this work M-C.L. was supported by the Waterloo Foundation, the Ministry of Education, Taiwan, Wolfson College, Cambridge, EU-AIMS, and the William Binks Autism Neuroscience Fellowship; M.V.L. by the Shirley Foundation, the Wellcome Trust, the British Academy, and Jesus College, Cambridge; B.C. by the UK Medical Research Council; S.B-C. by the Wellcome Trust, the UK Medical Research Council, the Waterloo Foundation, the Autism Research Trust, and EU-AIMS.