Whole-genome analysis of noncoding genetic variations identifies multiscale regulatory element perturbations associated with Hirschsprung disease

Whole-genome analysis of noncoding genetic variations identifies multiscale regulatory element perturbations associated with Hirschsprung disease

It is widely recognized that noncoding genetic variants play important roles in many human diseases, but there are multiple challenges that hinder the identification of functional disease-associated noncoding variants. The number of noncoding variants can be many times that of coding variants; many...

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Veröffentlicht in:Genome research 2020-11, Vol.30 (11), p.1618-1632
Hauptverfasser: Fu, Alexander Xi, Lui, Kathy Nga-Chu, Tang, Clara Sze-Man, Ng, Ray Kit, Lai, Frank Pui-Ling, Lau, Sin-Ting, Li, Zhixin, Garcia-Barcelo, Maria-Mercè, Sham, Pak-Chung, Tam, Paul Kwong-Hang, Ngan, Elly Sau-Wai, Yip, Kevin Y
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Sprache:eng
Schlagworte:
Disease
Epistasis
Gene regulation
Genetic analysis
Genetic diversity
Genomes
Gliogenesis
Hirschsprung's disease
Linkage disequilibrium
Method
Neural crest
Regulatory sequences
Whole genome sequencing
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container_end_page 1632
container_issue 11
container_start_page 1618
container_title Genome research
container_volume 30
creator Fu, Alexander Xi
Lui, Kathy Nga-Chu
Tang, Clara Sze-Man
Ng, Ray Kit
Lai, Frank Pui-Ling
Lau, Sin-Ting
Li, Zhixin
Garcia-Barcelo, Maria-Mercè
Sham, Pak-Chung
Tam, Paul Kwong-Hang
Ngan, Elly Sau-Wai
Yip, Kevin Y
description It is widely recognized that noncoding genetic variants play important roles in many human diseases, but there are multiple challenges that hinder the identification of functional disease-associated noncoding variants. The number of noncoding variants can be many times that of coding variants; many of them are not functional but in linkage disequilibrium with the functional ones; different variants can have epistatic effects; different variants can affect the same genes or pathways in different individuals; and some variants are related to each other not by affecting the same gene but by affecting the binding of the same upstream regulator. To overcome these difficulties, we propose a novel analysis framework that considers convergent impacts of different genetic variants on protein binding, which provides multiscale information about disease-associated perturbations of regulatory elements, genes, and pathways. Applying it to our whole-genome sequencing data of 918 short-segment Hirschsprung disease patients and matched controls, we identify various novel genes not detected by standard single-variant and region-based tests, functionally centering on neural crest migration and development. Our framework also identifies upstream regulators whose binding is influenced by the noncoding variants. Using human neural crest cells, we confirm cell stage-specific regulatory roles of three top novel regulatory elements on our list, respectively in the , , and loci. In the regulatory element, we further show that a noncoding variant found only in the patients affects the binding of the gliogenesis regulator NFIA, with a corresponding up-regulation of multiple genes in the same topologically associating domain.
doi_str_mv 10.1101/gr.264473.120
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Our framework also identifies upstream regulators whose binding is influenced by the noncoding variants. Using human neural crest cells, we confirm cell stage-specific regulatory roles of three top novel regulatory elements on our list, respectively in the , , and loci. In the regulatory element, we further show that a noncoding variant found only in the patients affects the binding of the gliogenesis regulator NFIA, with a corresponding up-regulation of multiple genes in the same topologically associating domain.</abstract><cop>United States</cop><pub>Cold Spring Harbor Laboratory Press</pub><pmid>32948616</pmid><doi>10.1101/gr.264473.120</doi><tpages>15</tpages><orcidid>https://orcid.org/0000-0001-5516-9944</orcidid><oa>free_for_read</oa></addata></record>
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subjects Disease
Epistasis
Gene regulation
Genetic analysis
Genetic diversity
Genomes
Gliogenesis
Hirschsprung's disease
Linkage disequilibrium
Method
Neural crest
Regulatory sequences
Whole genome sequencing
title Whole-genome analysis of noncoding genetic variations identifies multiscale regulatory element perturbations associated with Hirschsprung disease
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