Comprehensive functional genomic resource and integrative model for the human brain.

Daifeng Wang ,Tonya M Brunetti ,Shuang Liu ,Panos Roussos ,Selim Kalayci ,Xu Shi ,Kasidet Manakongtreecheep ,Mette A Peters ,Prashant S Emani ,Jonathan J Park ,Suhn Kyong Rhie ,Eugenio Mattei ,Fábio C P Navarro ,Holly Zhou ,Gabriel E Hoffman ,Zhiping Weng ,Michael J Gandal ,Declan Clarke ,Kiran Girdhar ,Jill E Moore ,Yu Yang ,Kevin P White ,Gregory E Crawford ,Shaoke Lou ,Nenad Šestan ,Mengting Gu ,Andrew E Jaffe ,Jonathan Warrell ,Chengfei Yan ,Daniel H Geschwind ,Yan Jiang ,Hyejung Won ,Min Xu ,Dominic Fitzgerald ,James A Knowles ,Zeynep H Gümüş ,Jing Zhang ,Schahram Akbarian ,Aparna Nathan ,Mark Gerstein

doi:10.1126/science.aat8464

Abstract

Despite progress in defining genetic risk for psychiatric disorders, their molecular mechanisms remain elusive. Addressing this, the PsychENCODE Consortium has generated a comprehensive online resource for the adult brain across 1866 individuals. The PsychENCODE resource contains ~79,000 brain-active enhancers, sets of Hi-C linkages, and topologically associating domains; single-cell expression profiles for many cell types; expression quantitative-trait loci (QTLs); and further QTLs associated with chromatin, splicing, and cell-type proportions. Integration shows that varying cell-type proportions largely account for the cross-population variation in expression (with >88% reconstruction accuracy). It also allows building of a gene regulatory network, linking genome-wide association study variants to genes (e.g., 321 for schizophrenia). We embed this network into an interpretable deep-learning model, which improves disease prediction by ~6-fold versus polygenic risk scores and identifies key genes and pathways in psychiatric disorders.

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