Roles of the BRD4 short isoform in phase separation and active gene transcription

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作者
Xinye Han
Di Yu
Ruirui Gu
Yanjie Jia
Qi Wang
Anbalagan Jaganathan
Xuelan Yang
Miaomiao Yu
Nicolas Babault
Chengcheng Zhao
Huanfa Yi
Qiang Zhang
Ming-Ming Zhou
Lei Zeng
机构
[1] Jilin University,Bethune Institute of Epigenetic Medicine, The First Hospital
[2] Jilin University,International Center of Future Science
[3] Icahn School of Medicine at Mount Sinai,Department of Pharmacological Sciences
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BRD4, a major tandem-bromodomain-containing transcription regulator, has two isoforms. The long isoform (BRD4L) has an extended C terminus that binds transcription cofactors, while the short isoform (BRD4S) lacks this C-terminal extension. Unlike BRD4L, the role of BRD4S in gene transcription remains unclear. Here, we report that, in human cancer cells, BRD4S forms nuclear puncta that possess liquid-like properties and that colocalize with BRD4L, MED1 and sites of histone H3 lysine 27 acetylation. BRD4 puncta are correlated with BRD4S but not BRD4L expression levels. BRD4S knockdown reduces BRD4S condensation, and ectopic expression promotes puncta formation and target gene transcription. BRD4S nuclear condensation is mediated by its intrinsically disordered regions and binding of its bromodomains to DNA and acetylated chromatin, respectively, and BRD4S phosphorylation diminishes BRD4 condensation. Our study illuminates a previously unappreciated role of BRD4S in organizing chromatin and transcription factors through phase separation to sustain gene transcription in chromatin for cancer cell proliferation.
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页码:333 / 341
页数:8
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