4.7 Article

Biological sex affects the neurobiology of autism

期刊

BRAIN
卷 136, 期 -, 页码 2799-2815

出版社

OXFORD UNIV PRESS
DOI: 10.1093/brain/awt216

关键词

autism; brain; sex differences; volumetric MRI

资金

  1. UK Medical Research Council [GO 400061]
  2. European Autism Interventions-A Multicentre Study for Developing New Medications (EU-AIMS)
  3. European Union [115300]
  4. Waterloo Foundation [921/1247]
  5. Ministry of Education, Taiwan
  6. Wellcome Trust
  7. British Academy
  8. Jesus College, Cambridge
  9. Autism Research Trust
  10. EFPIA
  11. Autism Speaks
  12. Medical Research Council [G0600977, G0001354B, G0001354, G1000183B, G0400061] Funding Source: researchfish
  13. National Institute for Health Research [RP-PG-0606-1045, NF-SI-0510-10268] Funding Source: researchfish
  14. MRC [G0400061, G0600977] Funding Source: UKRI

向作者/读者索取更多资源

In autism, heterogeneity is the rule rather than the exception. One obvious source of heterogeneity is biological sex. Since autism was first recognized, males with autism have disproportionately skewed research. Females with autism have thus been relatively overlooked, and have generally been assumed to have the same underlying neurobiology as males with autism. Growing evidence, however, suggests that this is an oversimplification that risks obscuring the biological base of autism. This study seeks to answer two questions about how autism is modulated by biological sex at the level of the brain: (i) is the neuroanatomy of autism different in males and females? and (ii) does the neuroanatomy of autism fit predictions from the 'extreme male brain' theory of autism, in males and/or in females? Neuroanatomical features derived from voxel-based morphometry were compared in a sample of equal-sized high-functioning male and female adults with and without autism (n = 120, n = 30/group). The first question was investigated using a 2 x 2 factorial design, and by spatial overlap analyses of the neuroanatomy of autism in males and females. The second question was tested through spatial overlap analyses of specific patterns predicted by the extreme male brain theory. We found that the neuroanatomy of autism differed between adult males and females, evidenced by minimal spatial overlap (not different from that occurred under random condition) in both grey and white matter, and substantially large white matter regions showing significant sex x diagnosis interactions in the 2 x 2 factorial design. These suggest that autism manifests differently by biological sex. Furthermore, atypical brain areas in females with autism substantially and non-randomly (P < 0.001) overlapped with areas that were sexually dimorphic in neurotypical controls, in both grey and white matter, suggesting neural 'masculinization'. This was not seen in males with autism. How differences in neuroanatomy relate to the similarities in cognition between males and females with autism remains to be understood. Future research should stratify by biological sex to reduce heterogeneity and to provide greater insight into the neurobiology of autism.

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