| Literature DB >> 34916619 |
Xianju Bi1, Yixuan Pan2, Boyang Gao1, Wen Shao1, Jun Wu2, Yafei Yin1, Zhimin Liu1, Mengyuan Peng2, Wenhao Zhang3, Xu Jiang3, Wenlin Ren1, Yanhui Xu1, Zhongyang Wu1, Kaili Wang1, Ge Zhan1, J Yuyang Lu1, Xue Han1, Tong Li1, Jianlong Wang4, Guohong Li5, Haiteng Deng3, Bing Li6, Xiaohua Shen7.
Abstract
An RNA-involved phase-separation model has been proposed for transcription control. However, the molecular links that connect RNA to the transcription machinery remain missing. Here we find that RNA-binding proteins (RBPs) constitute half of the chromatin proteome in embryonic stem cells (ESCs), some being colocalized with RNA polymerase (Pol) II at promoters and enhancers. Biochemical analyses of representative RBPs show that the paraspeckle protein PSPC1 inhibits the RNA-induced premature release of Pol II, and makes use of RNA as multivalent molecules to enhance the formation of transcription condensates and subsequent phosphorylation and release of Pol II. This synergistic interplay enhances polymerase engagement and activity via the RNA-binding and phase-separation activities of PSPC1. In ESCs, auxin-induced acute degradation of PSPC1 leads to genome-wide defects in Pol II binding and nascent transcription. We propose that promoter-associated RNAs and their binding proteins synergize the phase separation of polymerase condensates to promote active transcription.Entities:
Mesh:
Substances:
Year: 2021 PMID: 34916619 DOI: 10.1038/s41589-021-00904-5
Source DB: PubMed Journal: Nat Chem Biol ISSN: 1552-4450 Impact factor: 15.040