Genetic regulation of cell type-specific chromatin accessibility shapes brain disease etiology.

Biao Zeng,Biao Zeng,Biao Zeng,Biao Zeng,Panos Roussos,Chengyu Deng,Pavan Auluck,Panos Roussos,Panos Roussos,Jaroslav Bendl,Sarah M Reach,Ruth Misir,Jaroslav Bendl,David A Lewis,Gabriel E Hoffman,Nadav Ahituv,Vahram Haroutunian,Gabriel E Hoffman,Panos Roussos,Donghoon Lee,Stefano Marenco,John F Fullard,Steven P Kleopoulos,Vahram Haroutunian,Ruth Misir,Donghoon Lee,Gabriel E Hoffman,Steven P Kleopoulos,Jaroslav Bendl,Ruth Misir,Ruth Misir,Nadav Ahituv,Gabriel E Hoffman,Chengyu Deng,Sarah M Reach,Sarah M Reach,Steven P Kleopoulos,Donghoon Lee,John F Fullard,Sarah M Reach,Vahram Haroutunian,Panos Roussos,Donghoon Lee,Vahram Haroutunian,Jaroslav Bendl,John F Fullard,John F Fullard,Steven P Kleopoulos

doi:10.1126/science.adh4265

Abstract

Nucleotide variants in cell type-specific gene regulatory elements in the human brain are risk factors for human disease. We measured chromatin accessibility in 1932 aliquots of sorted neurons and non-neurons from 616 human postmortem brains and identified 34,539 open chromatin regions with chromatin accessibility quantitative trait loci (caQTLs). Only 10.4% of caQTLs are shared between neurons and non-neurons, which supports cell type-specific genetic regulation of the brain regulome. Incorporating allele-specific chromatin accessibility improves statistical fine-mapping and refines molecular mechanisms that underlie disease risk. Using massively parallel reporter assays in induced excitatory neurons, we screened 19,893 brain QTLs and identified the functional impact of 476 regulatory variants. Combined, this comprehensive resource captures variation in the human brain regulome and provides insights into disease etiology.

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