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A direct interaction between CPF and RNA Pol II links RNA 3′ end processing to transcription

Manuel Carminati, Juan B. Rodríguez‐Molina, M. Cemre Manav, Dom Bellini, Lori A. Passmore

2023Molecular Cell37 citationsDOIOpen Access PDF

Abstract

Transcription termination by RNA polymerase II (RNA Pol II) is linked to RNA 3' end processing by the cleavage and polyadenylation factor (CPF or CPSF). CPF contains endonuclease, poly(A) polymerase, and protein phosphatase activities, which cleave and polyadenylate pre-mRNAs and dephosphorylate RNA Pol II to control transcription. Exactly how the RNA 3' end processing machinery is coupled to transcription remains unclear. Here, we combine in vitro reconstitution, structural studies, and genome-wide analyses to show that yeast CPF physically and functionally interacts with RNA Pol II. Surprisingly, CPF-mediated dephosphorylation promotes the formation of an RNA Pol II stalk-to-stalk homodimer in vitro. This dimer is compatible with transcription but not with the binding of transcription elongation factors. Disruption of the dimerization interface in cells causes transcription defects, including altered RNA Pol II abundance on protein-coding genes, tRNA genes, and intergenic regions. We hypothesize that RNA Pol II dimerization may provide a mechanistic basis for the allosteric model of transcription termination.

Topics & Concepts

BiologyRNA polymerase IITranscription factor II DTranscription factor II FTranscription (linguistics)RNA polymerase II holoenzymeTranscription factor II BRNATermination factorGeneral transcription factorTranscription factor II EMolecular biologyRNA polymerase IIIPolyadenylationRNA-dependent RNA polymeraseRNA polymeraseCell biologyGeneticsGeneGene expressionPromoterLinguisticsPhilosophyRNA Research and SplicingGenomics and Chromatin DynamicsRNA and protein synthesis mechanisms