Human-lineage-specific genomic elements are associated with neurodegenerative disease and APOE transcript usage

Author:

Chen Zhongbo, ,Zhang David,Reynolds Regina H.ORCID,Gustavsson Emil K.ORCID,García-Ruiz Sonia,D’Sa Karishma,Fairbrother-Browne Aine,Vandrovcova Jana,Hardy John,Houlden HenryORCID,Gagliano Taliun Sarah A.ORCID,Botía Juan,Ryten MinaORCID

Abstract

AbstractKnowledge of genomic features specific to the human lineage may provide insights into brain-related diseases. We leverage high-depth whole genome sequencing data to generate a combined annotation identifying regions simultaneously depleted for genetic variation (constrained regions) and poorly conserved across primates. We propose that these constrained, non-conserved regions (CNCRs) have been subject to human-specific purifying selection and are enriched for brain-specific elements. We find that CNCRs are depleted from protein-coding genes but enriched within lncRNAs. We demonstrate that per-SNP heritability of a range of brain-relevant phenotypes are enriched within CNCRs. We find that genes implicated in neurological diseases have high CNCR density, including APOE, highlighting an unannotated intron-3 retention event. Using human brain RNA-sequencing data, we show the intron-3-retaining transcript to be more abundant in Alzheimer’s disease with more severe tau and amyloid pathological burden. Thus, we demonstrate potential association of human-lineage-specific sequences in brain development and neurological disease.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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