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Three decades of ASD genetics: building a foundation for neurobiological understanding and treatment
Author(s) -
Katherine W. Eyring,
Daniel H. Geschwind
Publication year - 2021
Publication title -
human molecular genetics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.811
H-Index - 276
eISSN - 1460-2083
pISSN - 0964-6906
DOI - 10.1093/hmg/ddab176
Subject(s) - biology , autism , exome sequencing , genomics , context (archaeology) , human genetics , genetics , genome wide association study , exome , genome , disease , autism spectrum disorder , computational biology , gene , mutation , single nucleotide polymorphism , developmental psychology , genotype , psychology , medicine , paleontology , pathology
Methodological advances over the last three decades have led to a profound transformation in our understanding of the genetic origins of neuropsychiatric disorders. This is exemplified by the study of autism spectrum disorders (ASDs) for which microarrays, whole exome sequencing and whole genome sequencing have yielded over a hundred causal loci. Genome-wide association studies in ASD have also been fruitful, identifying 5 genome-wide significant loci thus far and demonstrating a substantial role for polygenic inherited risk. Approaches rooted in systems biology and functional genomics have increasingly placed genes implicated by risk variants into biological context. Genetic risk affects a finite group of cell-types and biological processes, converging primarily on early stages of brain development (though, the expression of many risk genes persists through childhood). Coupled with advances in stem cell-based human in vitro model systems, these findings provide a basis for developing mechanistic models of disease pathophysiology.

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