Targeting transcription regulation in cancer with a covalent CDK7 inhibitor

Kwiatkowski, Nicholas; Zhang, Tinghu; Rahl, Peter B.; Abraham, Brian J.; Reddy, Josina C.; Ficarro, Scott B.; Dastur, Anahita; Amzallag, Arnaud; Ramaswamy, Sridhar; Tesar, Bethany; Jenkins, Christopher; Hannett, Nancy M.; McMillin, Douglas W.; Sanda, Takaomi; Sim, Taebo; Kim, Nam Doo; Look, A. Thomas; Mitsiades, Constantine S.; Weng, Andrew P.; Brown, Jennifer R.; Benes, Cyril H.; Marto, Jarrod A.; Young, Richard A.; Gray, Nathanael S.

doi:10.1038/nature13393

Cited by 728 publications

(1,027 citation statements)

References 30 publications

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“…1A). We next tested inhibitors of TFIIH CDK7 kinase activity (THZ) and the P-TEFb CDK9 inhibitor flavopiridol (FP) in our assay (47,48). Both THZ and flavopiridol have been shown previously to block transcription elongation in vitro (48,49).…”

Section: Oga Activity Is Required For Efficient Elongation In Vitro-mentioning

confidence: 99%

“…The full-length labeled RNA run-off product of 548 nucleotides is indicated by the arrow. THZ is an inhibitor of the CDK7 kinase subunit of TFIIH, and FP is a P-TEFb inhibitor (47,48). PUGNAc and Thiamet G were added after a 30 h PIC formation step as our previous work suggested that OGA might be required for PIC formation (43).…”

Section: Oga Activity Is Required For Efficient Elongation In Vitro-mentioning

confidence: 99%

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O-GlcNAcase Is an RNA Polymerase II Elongation Factor Coupled to Pausing Factors SPT5 and TIF1β

Resto

Kim

Fernandez

et al. 2016

Journal of Biological Chemistry

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We describe here the identification and functional characterization of the enzyme O-GlcNAcase (OGA) as an RNA polymerase II elongation factor. Using in vitro transcription elongation assays, we show that OGA activity is required for elongation in a crude nuclear extract system, whereas in a purified system devoid of OGA the addition of rOGA inhibited elongation. Furthermore, OGA is physically associated with the known RNA polymerase II (pol II) pausing/elongation factors SPT5 and TRIM28-KAP1-TIF1␤, and a purified OGA-SPT5-TIF1␤ complex has elongation properties. Lastly, ChIP-seq experiments show that OGA maps to the transcriptional start site/5 ends of genes, showing considerable overlap with RNA pol II, SPT5, TRIM28-KAP1-TIF1␤, and O-GlcNAc itself. These data all point to OGA as a component of the RNA pol II elongation machinery regulating elongation genome-wide. Our results add a novel and unexpected dimension to the regulation of elongation by the insertion of O-GlcNAc cycling into the pol II elongation regulatory dynamics.RNA polymerase II is the species of polymerase that transcribes the protein-coding genes in the cell. Largely based on in vitro transcription data and bacterial transcriptional regulation, it was thought that the pathway of transcription initiation was the de novo assembly and recruitment of general factors and pol II 4 into a preinitiation complex at promoters. In other words, transcription was solely controlled by whether initiation occurred or not. However, in the late 1980s, a transcriptionally engaged pol II was found on several genes, located roughly at ϩ50 relative to the transcriptional start site (TSS) (1-3). More recently, genome-wide approaches have shown that paused pol II exists on at least 40% of promoters in the genome (4 -9).These data show that the regulation of elongation is a significant and widespread method by which cells regulate gene expression.Biochemically, the establishment of a paused polymerase requires the recruitment of DSIF and NELF to pol II early in elongation to prevent pol II from productive elongation (10 -13). Release of the paused polymerase is achieved with P-TEFb phosphorylation of DSIF and NELF, ejecting NELF from pol II and converting DSIF into a positive elongation factor (14,15). The more recent discoveries of additional factors likely involved in pause establishment and release include human capping enzyme (16), the TFIIH-associated kinase, CDK7 (17, 18), the TFIIH ERCC3 helicase (19), , Integrator (23,24), ELL (25), TFIIS (26), TRIM28-KAP1-TIF1␤ (27, 28), Top1 (29), SEC (30), PAF complex (31, 32), and Gdown1 (33). The plethora of factors suggests that more complicated dynamics are at play in regulating pausing and elongation. Additionally, it is not clear, and indeed difficult to know, whether all of the factors involved in pol II pausing and elongation have been identified. This difficulty is due mostly to the absence of a human cell-based in vitro transcription system that recapitulates a paused polymerase and with which the full complement of...

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Section: Oga Activity Is Required For Efficient Elongation In Vitro-mentioning

confidence: 99%

Section: Oga Activity Is Required For Efficient Elongation In Vitro-mentioning

confidence: 99%

O-GlcNAcase Is an RNA Polymerase II Elongation Factor Coupled to Pausing Factors SPT5 and TIF1β

Resto

Kim

Fernandez

et al. 2016

Journal of Biological Chemistry

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“…Still, while CDK9 inhibition broadens the possibilities for ''anti-MYC'' therapy, its impact is not as great as MYC inhibition. Perhaps combinatorial therapies using the multikinase inhibitor sorafenib, a recently developed covalent CDK7 inhibitor that targets transcription regulation (Kwiatkowski et al 2014), or those targeting other MYC activities will synergize with CDK9 inhibition in producing strong anti-tumor effects.…”

Section: Discussionmentioning

confidence: 99%

CDK9-mediated transcription elongation is required for MYC addiction in hepatocellular carcinoma

et al. 2014

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One-year survival rates for newly diagnosed hepatocellular carcinoma (HCC) are <50%, and unresectable HCC carries a dismal prognosis owing to its aggressiveness and the undruggable nature of its main genetic drivers. By screening a custom library of shRNAs directed toward known drug targets in a genetically defined Myc-driven HCC model, we identified cyclin-dependent kinase 9 (Cdk9) as required for disease maintenance. Pharmacological or shRNA-mediated CDK9 inhibition led to robust anti-tumor effects that correlated with MYC expression levels and depended on the role that both CDK9 and MYC exert in transcription elongation. Our results establish CDK9 inhibition as a therapeutic strategy for MYC-overexpressing liver tumors and highlight the relevance of transcription elongation in the addiction of cancer cells to MYC.

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“…Indeed flavopiridol, a broad-acting kinase inhibitor that potently inhibits both CDK7 and CDK9 activity, has shown some promise in the treatment of several types of hematologic malignancies [15]. Recently, a drug prototype that is a remarkably selective inhibitor of CDK7 has been described [16]. This compound, THZ1, achieves relative selectivity for CDK7 through a covalent binding mechanism mediated by a reactive cysteine residue located outside the kinase pocket.…”

Section: Targeting Transcription Kinasesmentioning

confidence: 99%

Promising New Strategies to Target Gene Regulatory Factors in T-Cell Acute Lymphoblastic Leukemia

Ott¹

2014

Int. J. Hematol. Oncol.

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Targeting transcription regulation in cancer with a covalent CDK7 inhibitor

Cited by 728 publications

References 30 publications

O-GlcNAcase Is an RNA Polymerase II Elongation Factor Coupled to Pausing Factors SPT5 and TIF1β

O-GlcNAcase Is an RNA Polymerase II Elongation Factor Coupled to Pausing Factors SPT5 and TIF1β

CDK9-mediated transcription elongation is required for MYC addiction in hepatocellular carcinoma

Promising New Strategies to Target Gene Regulatory Factors in T-Cell Acute Lymphoblastic Leukemia

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