作者
Avik Choudhuri, Eirini Trompouki, Brian J Abraham, Leandro M Colli, Kian Hong Kock, William Mallard, Min-Lee Yang, Divya S Vinjamur, Alireza Ghamari, Audrey Sporrij, Karen Hoi, Barbara Hummel, Sonja Boatman, Victoria Chan, Sierra Tseng, Satish K Nandakumar, Song Yang, Asher Lichtig, Michael Superdock, Seraj N Grimes, Teresa V Bowman, Yi Zhou, Shinichiro Takahashi, Roby Joehanes, Alan B Cantor, Daniel E Bauer, Santhi K Ganesh, John Rinn, Paul S Albert, Martha L Bulyk, Stephen J Chanock, Richard A Young, Leonard I Zon
发表日期
2020/12
期刊
Nature genetics
卷号
52
期号
12
页码范围
1333-1345
出版商
Nature Publishing Group US
简介
Genome-wide association studies identify genomic variants associated with human traits and diseases. Most trait-associated variants are located within cell-type-specific enhancers, but the molecular mechanisms governing phenotypic variation are less well understood. Here, we show that many enhancer variants associated with red blood cell (RBC) traits map to enhancers that are co-bound by lineage-specific master transcription factors (MTFs) and signaling transcription factors (STFs) responsive to extracellular signals. The majority of enhancer variants reside on STF and not MTF motifs, perturbing DNA binding by various STFs (BMP/TGF-β-directed SMADs or WNT-induced TCFs) and affecting target gene expression. Analyses of engineered human blood cells and expression quantitative trait loci verify that disrupted STF binding leads to altered gene expression. Our results propose that the majority of the RBC …
学术搜索中的文章
A Choudhuri, E Trompouki, BJ Abraham, LM Colli… - Nature genetics, 2020