Mobile element variation contributes to population-specific genome diversification, gene regulation and disease risk.

Nature genetics
Authors
Shohei Kojima
Satoshi Koyama
Mirei Ka
Yuka Saito
Erica Parrish
Mikiko Endo
Sadaaki Takata
Misaki Mizukoshi
Keiko Hikino
Atsushi Takeda
Asami Gelinas
Steven Heaton
Rie Koide
Anselmo Kamada
Michiya Noguchi
Michiaki Hamada
Biobank Consortium
Yoichiro Kamatani
Yasuhiro Murakawa
Kazuyoshi Ishigaki
Yukio Nakamura
Kaoru Ito
Chikashi Terao
Yukihide Momozawa
Nicholas Parrish
Abstract

Mobile genetic elements (MEs) are heritable mutagens that recursively generate structural variants (SVs). ME variants (MEVs) are difficult to genotype and integrate in statistical genetics, obscuring their impact on genome diversification and traits. We developed a tool that accurately genotypes MEVs using short-read whole-genome sequencing (WGS) and applied it to global human populations. We find unexpected population-specific MEV differences, including an Alu insertion distribution distinguishing Japanese from other populations. Integrating MEVs with expression quantitative trait loci (eQTL) maps shows that MEV classes regulate tissue-specific gene expression by shared mechanisms, including creating or attenuating enhancers and recruiting post-transcriptional regulators, supporting class-wide interpretability. MEVs more often associate with gene expression changes than SNVs, thus plausibly impacting traits. Performing genome-wide association study (GWAS) with MEVs pinpoints potential causes of disease risk, including a LINE-1 insertion associated with keloid and fasciitis. This work implicates MEVs as drivers of human divergence and disease risk.
Year of Publication
2023
Journal
Nature genetics
Date Published
05/2023
ISSN
1546-1718
DOI
10.1038/s41588-023-01390-2
PubMed ID
37169872
Links

Recent Ó³»­´«Ã½ Publications