TY - JOUR
T1 - Brain-based sex differences in autism spectrum disorder across the lifespan
T2 - A systematic review of structural MRI, fMRI, and DTI findings
AU - Walsh, Melissa J.M.
AU - Wallace, Gregory L.
AU - Gallegos, Stephen M.
AU - Braden, B. Blair
N1 - Funding Information:
We thank our participants and the Submitters to the National Institute of Mental Health (NIMH) Data Archive (NDA) who made the analysis of sex differences in symptom severity age patterns in adolescents/adults possible. A portion of the data used in the preparation of this manuscript were obtained from the NIMH NDA. NDA is a collaborative informatics system created by the National Institutes of Health (NIH) to provide a national resource to support and accelerate research in mental health. Dataset identifier (10.15154/1522486). This manuscript reflects the views of the authors and may not reflect the opinions or views of the NIH or the Submitters submitting original data to NDA. The manuscript preparation was supported by the National Institute of Mental Health [NIMH; 1F31MH122107; 1K01MH116098]. The Social Responsiveness Scale – 2nd Edition data collected by our lab was supported by the NIMH [1K01MH116098], Department of Defense [AR140105], and Arizona Biomedical Research Commission [ADHS16-162413]. The funding sources had no involvement in the research or preparation of this article.
Funding Information:
The manuscript preparation was supported by the National Institute of Mental Health [NIMH; 1F31MH122107; 1K01MH116098]. The Social Responsiveness Scale – 2 nd Edition data collected by our lab was supported by the NIMH [1K01MH116098], Department of Defense [AR140105], and Arizona Biomedical Research Commission [ADHS16-162413]. The funding sources had no involvement in the research or preparation of this article.
Publisher Copyright:
© 2021 The Author(s)
PY - 2021/1
Y1 - 2021/1
N2 - Females with autism spectrum disorder (ASD) have been long overlooked in neuroscience research, but emerging evidence suggests they show distinct phenotypic trajectories and age-related brain differences. Sex-related biological factors (e.g., hormones, genes) may play a role in ASD etiology and have been shown to influence neurodevelopmental trajectories. Thus, a lifespan approach is warranted to understand brain-based sex differences in ASD. This systematic review on MRI-based sex differences in ASD was conducted to elucidate variations across the lifespan and inform biomarker discovery of ASD in females We identified articles through two database searches. Fifty studies met criteria and underwent integrative review. We found that regions expressing replicable sex-by-diagnosis differences across studies overlapped with regions showing sex differences in neurotypical cohorts. Furthermore, studies investigating age-related brain differences across a broad age-span suggest distinct neurodevelopmental patterns in females with ASD. Qualitative comparison across youth and adult studies also supported this hypothesis. However, many studies collapsed across age, which may mask differences. Furthermore, accumulating evidence supports the female protective effect in ASD, although only one study examined brain circuits implicated in “protection.” When synthesized with the broader literature, brain-based sex differences in ASD may come from various sources, including genetic and endocrine processes involved in brain “masculinization” and “feminization” across early development, puberty, and other lifespan windows of hormonal transition. Furthermore, sex-related biology may interact with peripheral processes, in particular the stress axis and brain arousal system, to produce distinct neurodevelopmental patterns in males and females with ASD. Future research on neuroimaging-based sex differences in ASD would benefit from a lifespan approach in well-controlled and multivariate studies. Possible relationships between behavior, sex hormones, and brain development in ASD remain largely unexamined.
AB - Females with autism spectrum disorder (ASD) have been long overlooked in neuroscience research, but emerging evidence suggests they show distinct phenotypic trajectories and age-related brain differences. Sex-related biological factors (e.g., hormones, genes) may play a role in ASD etiology and have been shown to influence neurodevelopmental trajectories. Thus, a lifespan approach is warranted to understand brain-based sex differences in ASD. This systematic review on MRI-based sex differences in ASD was conducted to elucidate variations across the lifespan and inform biomarker discovery of ASD in females We identified articles through two database searches. Fifty studies met criteria and underwent integrative review. We found that regions expressing replicable sex-by-diagnosis differences across studies overlapped with regions showing sex differences in neurotypical cohorts. Furthermore, studies investigating age-related brain differences across a broad age-span suggest distinct neurodevelopmental patterns in females with ASD. Qualitative comparison across youth and adult studies also supported this hypothesis. However, many studies collapsed across age, which may mask differences. Furthermore, accumulating evidence supports the female protective effect in ASD, although only one study examined brain circuits implicated in “protection.” When synthesized with the broader literature, brain-based sex differences in ASD may come from various sources, including genetic and endocrine processes involved in brain “masculinization” and “feminization” across early development, puberty, and other lifespan windows of hormonal transition. Furthermore, sex-related biology may interact with peripheral processes, in particular the stress axis and brain arousal system, to produce distinct neurodevelopmental patterns in males and females with ASD. Future research on neuroimaging-based sex differences in ASD would benefit from a lifespan approach in well-controlled and multivariate studies. Possible relationships between behavior, sex hormones, and brain development in ASD remain largely unexamined.
KW - Autism spectrum disorder
KW - Brain
KW - Development
KW - MRI
KW - Neuroimaging
KW - Sex
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U2 - 10.1016/j.nicl.2021.102719
DO - 10.1016/j.nicl.2021.102719
M3 - Article
C2 - 34153690
AN - SCOPUS:85109165137
SN - 2213-1582
VL - 31
JO - NeuroImage: Clinical
JF - NeuroImage: Clinical
M1 - 102719
ER -