4.8 Article

Comprehensive RNA Polymerase II Interactomes Reveal Distinct and Varied Roles for Each Phospho-CTD Residue

Journal

CELL REPORTS
Volume 15, Issue 10, Pages 2147-2158

Publisher

CELL PRESS
DOI: 10.1016/j.celrep.2016.05.010

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Funding

  1. U.S. National Institutes of Health NHGRI grants [R01HG007173]
  2. Damon Runyon Dale F. Frey Award for Breakthrough Scientists
  3. Burroughs Wellcome Fund Career Award at the Scientific Interface
  4. U.S. National Science Foundation Graduate Research Fellowship [DGE1144152]

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Transcription controls splicing and other gene regulatory processes, yet mechanisms remain obscure due to our fragmented knowledge of the molecular connections between the dynamically phosphorylated RNA polymerase II (Pol II) C-terminal domain (CTD) and regulatory factors. By systematically isolating phosphorylation states of the CTD heptapeptide repeat (Y1S2P3T4S5P6S7), we identify hundreds of protein factors that are differentially enriched, revealing unappreciated connections between the Pol II CTD and co-transcriptional processes. These data uncover a role for threonine-4 in 30 end processing through control of the transition between cleavage and termination. Furthermore, serine-5 phosphorylation seeds spliceosomal assembly immediately downstream of 30 splice sites through a direct interaction with spliceosomal sub-complex U1. Strikingly, threonine-4 phosphorylation also impacts splicing by serving as a mark of co-transcriptional spliceosome release and ensuring efficient post-transcriptional splicing genome-wide. Thus, comprehensive Pol II interactomes identify the complex and functional connections between transcription machinery and other gene regulatory complexes.

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