Authors
Zuyao Ni, Chao Xu, Xinghua Guo, Gerald O Hunter, Olga V Kuznetsova, Wolfram Tempel, Edyta Marcon, Guoqing Zhong, Hongbo Guo, Wei-Hung William Kuo, Joyce Li, Peter Young, Jonathan B Olsen, Cuihong Wan, Peter Loppnau, Majida El Bakkouri, Guillermo A Senisterra, Hao He, Haiming Huang, Sachdev S Sidhu, Andrew Emili, Shona Murphy, Amber L Mosley, Cheryl H Arrowsmith, Jinrong Min, Jack F Greenblatt
Publication date
2014/8
Journal
Nature structural & molecular biology
Volume
21
Issue
8
Pages
686-695
Publisher
Nature Publishing Group US
Description
The RNA polymerase II (RNAPII) C-terminal domain (CTD) heptapeptide repeats (1-YSPTSPS-7) undergo dynamic phosphorylation and dephosphorylation during the transcription cycle to recruit factors that regulate transcription, RNA processing and chromatin modification. We show here that RPRD1A and RPRD1B form homodimers and heterodimers through their coiled-coil domains and interact preferentially via CTD-interaction domains (CIDs) with RNAPII CTD repeats phosphorylated at S2 and S7. Crystal structures of the RPRD1A, RPRD1B and RPRD2 CIDs, alone and in complex with RNAPII CTD phosphoisoforms, elucidate the molecular basis of CTD recognition. In an example of cross-talk between different CTD modifications, our data also indicate that RPRD1A and RPRD1B associate directly with RPAP2 phosphatase and, by interacting with CTD repeats where phospho-S2 and/or phospho-S7 bracket …
Scholar articles
RPRD1A and RPRD1B are human RNA polymerase II C-terminal domain scaffolds for Ser5 dephosphorylation
Z Ni, C Xu, X Guo, GO Hunter, OV Kuznetsova… - Nature structural & molecular biology, 2014