Braincharting autism and ADHD reveals age- and sex- specific effects
Presented During:
Tuesday, June 25, 2024: 12:00 PM - 1:15 PM
COEX
Room:
Hall D 2
Poster No:
396
Submission Type:
Abstract Submission
Authors:
Saashi Bedford1, Meng-Chuan Lai2, Michael Lombardo3, Bhismadev Chakrabarti4, Amber Ruigrok5, John Suckling6, Evdokia Anagnostou7, Jason Lerch8, Margot Taylor9, Rob Nicolson10, Georgiades Stelios11, Jennifer Crosbie12, Russell Schachar9, Elizabeth Kelley13, Jessica Jones13, Paul Arnold14, Eric Courchesne15, Karen Pierce16, Lisa Eyler17, Kathleen Campbell16, Cynthia Carter Barnes16, Jakob Seidlitz18, Aaron Alexander-Bloch18, Edward Bullmore6, Simon Baron-Cohen6, Richard Bethlehem19
Institutions:
1University of Cambridge, Cambridge, Select State/Province, 2Centre for Addiction and Mental Health, Toronto, Ontario, 3Laboratory for Autism and Neurodevelopmental Disorders, Istituto Italiano di Tecnologia, Rovereto, Italy, 4University of Reading, Reading, Berkshire, 5University of Manchester, Manchester, Lancashire, 6University of Cambridge, Cambridge, United Kingdom, 7University of Toronto, Toronto, Ontario, 8Wellcome Centre for Integrative Neuroimaging, University of Oxford, Oxford, Oxford, 9Hospital for Sick Children, Toronto, Ontario, 10University of Western Ontario, London, Ontario, 11McMaster University, Hamilton, Ontario, 12The Hospital for Sick Children, Toronto, Ontario, 13Queen’s University, Kingston, Kingston, Ontario, 14University of Calgary, Calgary, Alberta, 15University of California San Diego, San Diego, CA, 16University of California San Diego, San Diego, California, 17University of California San Diego, La Jolla, CA, 18University of Pennsylvania, Philadelphia, PA, 19Autism Research Centre, Department of Psychiatry, University of Cambridge, Cambridge, United Kingdom
First Author:
Co-Author(s):
Michael Lombardo
Laboratory for Autism and Neurodevelopmental Disorders, Istituto Italiano di Tecnologia
Rovereto, Italy
Laboratory for Autism and Neurodevelopmental Disorders, Istituto Italiano di Tecnologia
Rovereto, Italy
Richard Bethlehem
Autism Research Centre, Department of Psychiatry, University of Cambridge
Cambridge, United Kingdom
Autism Research Centre, Department of Psychiatry, University of Cambridge
Cambridge, United Kingdom
Introduction:
Autism and attention-deficit/hyperactivity disorder (ADHD) are heterogeneous neurodevelopmental conditions with complex underlying neurobiology, and neuroanatomical alterations have been reported in both [1–3]. Both conditions show significant sex and age modulations on neuroanatomy [3,4], which are not yet fully understood. Normative modelling is an emerging technique that provides a unified framework for studying age- and sex-specific divergence in brain development in a common space [5]. We aimed to characterise regional cortical and global neuroanatomy in autism and ADHD, as well as sex and age differences, benchmarked against models of typical brain development based on a sample of over 75,000 individuals.
Methods:
We combined T1-weighted MRIs from 49 sites across 7 datasets, for a total dataset of 4255 participants after quality control (1869 controls, 987 ADHD, 1399 autism; ages 2-64 years). Images were processed using FreeSurfer [6] 6.0.1, and regional cortical estimates extracted based on the Desikan-Killiany [7] atlas, for cortical thickness (CT), volume (CV) and surface area (SA). We also examined total grey and white matter volume, subcortical grey matter volume, ventricular volume, mean CT and total SA.
We used normative reference models [8] previously generated by our group to map neuroanatomical developmental trajectories across the lifespan for global and regional neuroanatomical measures, accounting for age, sex and site/scanner. Out-of-sample normative centile scores for our study sample were generated based on these models, quantifying divergence from normative brain development in our sample. We examined diagnostic group differences in centile scores, and the interaction between diagnosis and sex, for all global volumes and regional cortical measures using multiple linear regressions.
To examine age differences, we conducted a sliding-window age analysis to examine diagnostic group differences across development, in age intervals of 5 years, starting at 2 years and sliding by 1 year. We selected a random subset of 70 participants per group, bootstrapped 1000 times, and examined diagnostic group differences at each age interval, averaged across the 1000 bootstraps. This allowed us to determine change in group differences across development, and the age window with the maximum diagnostic group difference.
We used normative reference models [8] previously generated by our group to map neuroanatomical developmental trajectories across the lifespan for global and regional neuroanatomical measures, accounting for age, sex and site/scanner. Out-of-sample normative centile scores for our study sample were generated based on these models, quantifying divergence from normative brain development in our sample. We examined diagnostic group differences in centile scores, and the interaction between diagnosis and sex, for all global volumes and regional cortical measures using multiple linear regressions.
To examine age differences, we conducted a sliding-window age analysis to examine diagnostic group differences across development, in age intervals of 5 years, starting at 2 years and sliding by 1 year. We selected a random subset of 70 participants per group, bootstrapped 1000 times, and examined diagnostic group differences at each age interval, averaged across the 1000 bootstraps. This allowed us to determine change in group differences across development, and the age window with the maximum diagnostic group difference.
Results:
All results were significant at 5% false discovery rate. For global measures, individuals with ADHD had significantly lower total cortical and subcortical grey and white matter volumes, and total cortical SA centile scores (d = -0.13- -0.18), but greater mean CT centiles (d = 0.09) relative to controls. Autistic individuals had significantly larger ventricular volume centiles relative to controls (d = 0.15). Individuals with ADHD showed regional CT increases (d = 0.09-0.10) but lower CV and SA centiles (d = -0.07- -0.18) across much of the cortex. Autistic individuals showed greater regional CT and CV localised to the superior temporal cortex (STG; d = 0.13-0.15). There was a significant sex-by-diagnosis interaction, and distinct diagnostic differences by sex for autism, but not for ADHD, where autistic males had greater CV and CT in the STG, but autistic females had lower SA in the fusiform gyrus, relative to controls.
For autism, diagnostic group differences for the STG were strongest in the youngest age windows, across all cortical measures. For SA, and to a slightly less extent CV, this was also the case in most frontal and parietal regions. For CT, most other regions had the strongest effects in later ages, around 15-20 years. Group differences in ADHD were typically strongest at the latest age windows, starting at 14-15 years of age. Some regions showed the strongest differences in the youngest windows, including the STG for SA, and some frontal and parietal areas.
For autism, diagnostic group differences for the STG were strongest in the youngest age windows, across all cortical measures. For SA, and to a slightly less extent CV, this was also the case in most frontal and parietal regions. For CT, most other regions had the strongest effects in later ages, around 15-20 years. Group differences in ADHD were typically strongest at the latest age windows, starting at 14-15 years of age. Some regions showed the strongest differences in the youngest windows, including the STG for SA, and some frontal and parietal areas.
·Diagnostic and age differences in cortical measures related to autism and ADHD
·Sex differences in cortical measures related to autism and ADHD
Conclusions:
These results indicate distinct cortical differences in autism and ADHD that are differentially impacted by age and sex.
Disorders of the Nervous System:
Neurodevelopmental/ Early Life (eg. ADHD, autism) 1
Neuroanatomy, Physiology, Metabolism and Neurotransmission:
Cortical Anatomy and Brain Mapping 2
Keywords:
Attention Deficit Disorder
Autism
Computational Neuroscience
Cortex
Development
DISORDERS
MRI
Open Data
Psychiatric
STRUCTURAL MRI
1|2Indicates the priority used for review
Provide references using author date format
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