Tissue-specific BMAL1 cistromes reveal that rhythmic transcription is associated with rhythmic enhancer–enhancer interactions

Author:

Beytebiere Joshua R.,Trott Alexandra J.,Greenwell Ben J.,Osborne Collin A.,Vitet Helene,Spence Jessica,Yoo Seung-Hee,Chen Zheng,Takahashi Joseph S.,Ghaffari Noushin,Menet Jerome S.

Abstract

The mammalian circadian clock relies on the transcription factor CLOCK:BMAL1 to coordinate the rhythmic expression of thousands of genes. Consistent with the various biological functions under clock control, rhythmic gene expression is tissue-specific despite an identical clockwork mechanism in every cell. Here we show that BMAL1 DNA binding is largely tissue-specific, likely because of differences in chromatin accessibility between tissues and cobinding of tissue-specific transcription factors. Our results also indicate that BMAL1 ability to drive tissue-specific rhythmic transcription is associated with not only the activity of BMAL1-bound enhancers but also the activity of neighboring enhancers. Characterization of physical interactions between BMAL1 enhancers and other cis-regulatory regions by RNA polymerase II chromatin interaction analysis by paired-end tag (ChIA-PET) reveals that rhythmic BMAL1 target gene expression correlates with rhythmic chromatin interactions. These data thus support that much of BMAL1 target gene transcription depends on BMAL1 capacity to rhythmically regulate a network of enhancers.

Funder

Texas A&M University

National Institute of General Medical Sciences

Robert A. Welch Foundation

National Institute on Aging

Publisher

Cold Spring Harbor Laboratory

Subject

Developmental Biology,Genetics

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