The PP2A-Integrator-CDK9 axis fine-tunes transcription and can be targeted therapeutically in cancer | Zendy

Stephin J. Vervoort | Zendy; Sarah A. Welsh | Zendy; Jennifer R. Devlin | Zendy; Elisa Barbieri | Zendy; Deborah A. Knight | Zendy; Sarah Offley | Zendy; Stefan Bjelosevic | Zendy; Matteo Costacurta | Zendy; Izabela Todorovski | Zendy; Conor J. Kearney | Zendy; Jarrod J. Sandow | Zendy; Zheng Fan | Zendy; Benjamin J. Blyth | Zendy; Victoria M. McLeod | Zendy; Joseph H.A. Vissers | Zendy; Karolina Pavic | Zendy; Ben P. Martin | Zendy; Gareth P. Gregory | Zendy; Elena Demosthenous | Zendy; Magnus Zethoven | Zendy; Isabella Y. Kong | Zendy; Edwin D. Hawkins | Zendy; Simon J. Hogg | Zendy; Madison J. Kelly | Zendy; Andrea Newbold | Zendy; Kaylene J. Simpson | Zendy; Otto Kauko | Zendy; Kieran F. Harvey | Zendy; Michael Ohlmeyer | Zendy; Jukka Westermarck | Zendy; Nathanael S. Gray | Zendy; Alessandro Gardini | Zendy; Ricky W. Johnstone | Zendy

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The PP2A-Integrator-CDK9 axis fine-tunes transcription and can be targeted therapeutically in cancer

Author(s) -

Stephin J. Vervoort,

Sarah A. Welsh,

Jennifer R. Devlin,

Elisa Barbieri,

Deborah A. Knight,

Sarah Offley,

Stefan Bjelosevic,

Matteo Costacurta,

Izabela Todorovski,

Conor J. Kearney,

Jarrod J. Sandow,

Zheng Fan,

Benjamin J. Blyth,

Victoria M. McLeod,

Joseph H.A. Vissers,

Karolina Pavic,

Ben P. Martin,

Gareth P. Gregory,

Elena Demosthenous,

Magnus Zethoven,

Isabella Y. Kong,

Edwin D. Hawkins,

Simon J. Hogg,

Madison J. Kelly,

Andrea Newbold,

Kaylene J. Simpson,

Otto Kauko,

Kieran F. Harvey,

Michael Ohlmeyer,

Jukka Westermarck,

Nathanael S. Gray,

Alessandro Gardini,

Ricky W. Johnstone

Publication year - 2021

Publication title -

cell

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 26.304

H-Index - 776

eISSN - 1097-4172

pISSN - 0092-8674

DOI - 10.1016/j.cell.2021.04.022

Subject(s) - rna polymerase ii , biology , protein phosphatase 2 , cyclin dependent kinase , transcription (linguistics) , microbiology and biotechnology , cyclin dependent kinase 9 , kinase , cancer research , transcription factor , brd4 , phosphatase , gene expression , cell cycle , phosphorylation , protein kinase a , cyclin dependent kinase 2 , promoter , gene , biochemistry , bromodomain , histone , linguistics , philosophy

Gene expression by RNA polymerase II (RNAPII) is tightly controlled by cyclin-dependent kinases (CDKs) at discrete checkpoints during the transcription cycle. The pausing checkpoint following transcription initiation is primarily controlled by CDK9. We discovered that CDK9-mediated, RNAPII-driven transcription is functionally opposed by a protein phosphatase 2A (PP2A) complex that is recruited to transcription sites by the Integrator complex subunit INTS6. PP2A dynamically antagonizes phosphorylation of key CDK9 substrates including DSIF and RNAPII-CTD. Loss of INTS6 results in resistance to tumor cell death mediated by CDK9 inhibition, decreased turnover of CDK9 phospho-substrates, and amplification of acute oncogenic transcriptional responses. Pharmacological PP2A activation synergizes with CDK9 inhibition to kill both leukemic and solid tumor cells, providing therapeutic benefit in vivo. These data demonstrate that fine control of gene expression relies on the balance between kinase and phosphatase activity throughout the transcription cycle, a process dysregulated in cancer that can be exploited therapeutically.

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