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Covalent targeting of remote cysteine residues to develop CDK12 and CDK13 inhibitors

dc.contributor.authorZhang, Tinghu
dc.contributor.authorKwiatkowski, Nicholas
dc.contributor.authorOlson, Calla M
dc.contributor.authorDixon-Clarke, Sarah E
dc.contributor.authorAbraham, Brian J
dc.contributor.authorGreifenberg, Ann K
dc.contributor.authorFicarro, Scott B
dc.contributor.authorElkins, Jonathan M
dc.contributor.authorLiang, Yanke
dc.contributor.authorHannett, Nancy M
dc.contributor.authorManz, Theresa
dc.contributor.authorHao, Mingfeng
dc.contributor.authorBartkowiak, Bartlomiej
dc.contributor.authorGreenleaf, Arno L
dc.contributor.authorMarto, Jarrod A
dc.contributor.authorGeyer, Matthias
dc.contributor.authorBullock, Alex N
dc.contributor.authorGray, Nathanael S
dc.contributor.authorYoung, Richard A.
dc.date.accessioned2017-05-01T17:59:22Z
dc.date.available2017-05-01T17:59:22Z
dc.date.issued2016-08
dc.date.submitted2015-08
dc.identifier.issn1552-4450
dc.identifier.issn1552-4469
dc.identifier.urihttp://hdl.handle.net/1721.1/108541
dc.description.abstractCyclin-dependent kinases 12 and 13 (CDK12 and CDK13) play critical roles in the regulation of gene transcription. However, the absence of CDK12 and CDK13 inhibitors has hindered the ability to investigate the consequences of their inhibition in healthy cells and cancer cells. Here we describe the rational design of a first-in-class CDK12 and CDK13 covalent inhibitor, THZ531. Co-crystallization of THZ531 with CDK12–cyclin K indicates that THZ531 irreversibly targets a cysteine located outside the kinase domain. THZ531 causes a loss of gene expression with concurrent loss of elongating and hyperphosphorylated RNA polymerase II. In particular, THZ531 substantially decreases the expression of DNA damage response genes and key super-enhancer-associated transcription factor genes. Coincident with transcriptional perturbation, THZ531 dramatically induced apoptotic cell death. Small molecules capable of specifically targeting CDK12 and CDK13 may thus help identify cancer subtypes that are particularly dependent on their kinase activities.en_US
dc.description.sponsorshipUnited States. National Institutes of Health (HG002668)en_US
dc.description.sponsorshipUnited States. National Institutes of Health (CA109901)en_US
dc.language.isoen_US
dc.publisherNature Publishing Groupen_US
dc.relation.isversionofhttp://dx.doi.org/10.1038/nchembio.2166en_US
dc.rightsArticle is made available in accordance with the publisher's policy and may be subject to US copyright law. Please refer to the publisher's site for terms of use.en_US
dc.sourcePMCen_US
dc.titleCovalent targeting of remote cysteine residues to develop CDK12 and CDK13 inhibitorsen_US
dc.typeArticleen_US
dc.identifier.citationZhang, Tinghu; Kwiatkowski, Nicholas; Olson, Calla M; Dixon-Clarke, Sarah E; Abraham, Brian J; Greifenberg, Ann K and Ficarro, Scott B et al. “Covalent Targeting of Remote Cysteine Residues to Develop CDK12 and CDK13 Inhibitors.” Nature Chemical Biology 12, no. 10 (August 2016): 876–884. © 2016 Nature America, Incen_US
dc.contributor.departmentMassachusetts Institute of Technology. Department of Biologyen_US
dc.contributor.mitauthorYoung, Richard A
dc.relation.journalNature Chemical Biologyen_US
dc.eprint.versionAuthor's final manuscripten_US
dc.type.urihttp://purl.org/eprint/type/JournalArticleen_US
eprint.statushttp://purl.org/eprint/status/PeerRevieweden_US
dspace.orderedauthorsZhang, Tinghu; Kwiatkowski, Nicholas; Olson, Calla M; Dixon-Clarke, Sarah E; Abraham, Brian J; Greifenberg, Ann K; Ficarro, Scott B; Elkins, Jonathan M; Liang, Yanke; Hannett, Nancy M; Manz, Theresa; Hao, Mingfeng; Bartkowiak, Bartlomiej; Greenleaf, Arno L; Marto, Jarrod A; Geyer, Matthias; Bullock, Alex N; Young, Richard A; Gray, Nathanael Sen_US
dspace.embargo.termsNen_US
dc.identifier.orcidhttps://orcid.org/0000-0001-8855-8647
mit.licensePUBLISHER_POLICYen_US
mit.metadata.statusComplete


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