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SHARE-seq reveals chromatin potential

Authors :
Vinay K. Kartha
Lindsay M. LaFave
Alison Brack
Yan Hu
Ya-Chieh Hsu
Caleb A. Lareau
Travis Law
Jiarui Ding
Aviv Regev
Zachary Chiang
Sai Ma
Andrew S. Earl
Tristan Tay
Jason D. Buenrostro
Bing Zhang
Source :
Cell, PMC
Publication Year :
2020

Abstract

© 2020 Elsevier Inc. Cell differentiation and function are regulated across multiple layers of gene regulation, including modulation of gene expression by changes in chromatin accessibility. However, differentiation is an asynchronous process precluding a temporal understanding of regulatory events leading to cell fate commitment. Here we developed simultaneous high-throughput ATAC and RNA expression with sequencing (SHARE-seq), a highly scalable approach for measurement of chromatin accessibility and gene expression in the same single cell, applicable to different tissues. Using 34,774 joint profiles from mouse skin, we develop a computational strategy to identify cis-regulatory interactions and define domains of regulatory chromatin (DORCs) that significantly overlap with super-enhancers. During lineage commitment, chromatin accessibility at DORCs precedes gene expression, suggesting that changes in chromatin accessibility may prime cells for lineage commitment. We computationally infer chromatin potential as a quantitative measure of chromatin lineage-priming and use it to predict cell fate outcomes. SHARE-seq is an extensible platform to study regulatory circuitry across diverse cells in tissues.

Details

ISSN :
14710064
Volume :
22
Issue :
1
Database :
OpenAIRE
Journal :
Nature reviews. GeneticsOriginal article
Accession number :
edsair.doi.dedup.....a581afabe474bcec15c9d9e128afae97