Autism Spectrum Disorder: A Neuro-Immunometabolic Hypothesis of the Developmental Origins

Martin G Frasch; Byung-Jun Yoon; Dario Lucas Helbing; Gal Snir; Marta C Antonelli; Reinhard Bauer

doi:10.3390/biology12070914

Autism Spectrum Disorder: A Neuro-Immunometabolic Hypothesis of the Developmental Origins

Biology (Basel). 2023 Jun 26;12(7):914. doi: 10.3390/biology12070914.

Authors

Martin G Frasch^{1

2}, Byung-Jun Yoon³, Dario Lucas Helbing^{4

5

6

7}, Gal Snir¹, Marta C Antonelli^{8

9}, Reinhard Bauer⁴

Affiliations

¹ Department of Obstetrics and Gynecology, University of Washington, Seattle, WA 98195, USA.
² Center on Human Development and Disability, University of Washington, Seattle, WA 98195, USA.
³ Electrical and Computer Engineering, Texas A&M University, College Station, TX 77843, USA.
⁴ Institute for Molecular Cell Biology, Jena University Hospital, Friedrich Schiller University, 07747 Jena, Germany.
⁵ Leibniz Institute on Aging, Fritz Lipmann Institute, 07745 Jena, Germany.
⁶ Department of Psychiatry and Psychotherapy, Jena University Hospital, Friedrich Schiller University Jena, 07747 Jena, Germany.
⁷ Center for Intervention and Research on Adaptive and Maladaptive Brain Circuits Underlying Mental Health (C-I-R-C), Jena-Magdeburg-Halle, 07743 Jena, Germany.
⁸ Instituto de Biología Celular y Neurociencia "Prof. Eduardo De Robertis", Facultad de Medicina, Universidad de Buenos Aires, Buenos Aires 1121, Argentina.
⁹ Institute for Advanced Study, Technical University of Munich, Lichtenbergstrasse 2 a, 85748 Garching, Germany.

Abstract

Fetal neuroinflammation and prenatal stress (PS) may contribute to lifelong neurological disabilities. Astrocytes and microglia, among the brain's non-neuronal "glia" cell populations, play a pivotal role in neurodevelopment and predisposition to and initiation of disease throughout lifespan. One of the most common neurodevelopmental disorders manifesting between 1-4 years of age is the autism spectrum disorder (ASD). A pathological glial-neuronal interplay is thought to increase the risk for clinical manifestation of ASD in at-risk children, but the mechanisms remain poorly understood, and integrative, multi-scale models are needed. We propose a model that integrates the data across the scales of physiological organization, from genome to phenotype, and provides a foundation to explain the disparate findings on the genomic level. We hypothesize that via gene-environment interactions, fetal neuroinflammation and PS may reprogram glial immunometabolic phenotypes that impact neurodevelopment and neurobehavior. Drawing on genomic data from the recently published series of ovine and rodent glial transcriptome analyses with fetuses exposed to neuroinflammation or PS, we conducted an analysis on the Simons Foundation Autism Research Initiative (SFARI) Gene database. We confirmed 21 gene hits. Using unsupervised statistical network analysis, we then identified six clusters of probable protein-protein interactions mapping onto the immunometabolic and stress response networks and epigenetic memory. These findings support our hypothesis. We discuss the implications for ASD etiology, early detection, and novel therapeutic approaches. We conclude with delineation of the next steps to verify our model on the individual gene level in an assumption-free manner. The proposed model is of interest for the multidisciplinary community of stakeholders engaged in ASD research, the development of novel pharmacological and non-pharmacological treatments, early prevention, and detection as well as for policy makers.

Keywords: autism spectrum disorder; genomics; information theory; multi-scale modeling.

Grants and funding

This research received no external funding.