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Literature DB >> 33753926

Discovery and resistance mechanism of a selective CDK12 degrader.

Baishan Jiang^1,2, Yang Gao^1,2, Jianwei Che^1,2, Wenchao Lu^1,2, Ines H Kaltheuner³, Ruben Dries^4,5, Marian Kalocsay⁶, Matthew J Berberich⁶, Jie Jiang^1,2, Inchul You^1,2, Nicholas Kwiatkowski^1,2, Kristin M Riching⁷, Danette L Daniels⁷, Peter K Sorger⁶, Matthias Geyer³, Tinghu Zhang^8,9, Nathanael S Gray^10,11.

Abstract

Cyclin-dependent kinase 12 (CDK12) is an emerging therapeutic target due to its role in regulating transcription of DNA-damage response (DDR) genes. However, development of selective small molecules targeting CDK12 has been challenging due to the high degree of homology between kinase domains of CDK12 and other transcriptional CDKs, most notably CDK13. In the present study, we report the rational design and characterization of a CDK12-specific degrader, BSJ-4-116. BSJ-4-116 selectively degraded CDK12 as assessed through quantitative proteomics. Selective degradation of CDK12 resulted in premature cleavage and poly(adenylation) of DDR genes. Moreover, BSJ-4-116 exhibited potent antiproliferative effects, alone and in combination with the poly(ADP-ribose) polymerase inhibitor olaparib, as well as when used as a single agent against cell lines resistant to covalent CDK12 inhibitors. Two point mutations in CDK12 were identified that confer resistance to BSJ-4-116, demonstrating a potential mechanism that tumor cells can use to evade bivalent degrader molecules.

Entities: Chemical

Mesh：

Substances：

Year: 2021 PMID： 33753926 PMCID： PMC8590456 DOI： 10.1038/s41589-021-00765-y

Source DB: PubMed Journal: Nat Chem Biol ISSN： 1552-4450 Impact factor: 15.040

49 in total

1. Three RNA polymerase II carboxyl-terminal domain kinases display distinct substrate preferences.

Authors: Y Ramanathan; S M Rajpara; S M Reza; E Lees; S Shuman; M B Mathews; T Pe'ery
Journal: J Biol Chem Date: 2001-01-16 Impact factor: 5.157

Review 2. Secrets of a double agent: CDK7 in cell-cycle control and transcription.

Authors: Robert P Fisher
Journal: J Cell Sci Date: 2005-11-15 Impact factor: 5.285

3. EWS/FLI Confers Tumor Cell Synthetic Lethality to CDK12 Inhibition in Ewing Sarcoma.

Authors: Amanda Balboni Iniguez; Björn Stolte; Emily Jue Wang; Amy Saur Conway; Gabriela Alexe; Neekesh V Dharia; Nicholas Kwiatkowski; Tinghu Zhang; Brian J Abraham; Jaume Mora; Peter Kalev; Alan Leggett; Dipanjan Chowdhury; Cyril H Benes; Richard A Young; Nathanael S Gray; Kimberly Stegmaier
Journal: Cancer Cell Date: 2018-01-18 Impact factor: 31.743

4. CDK12 is a transcription elongation-associated CTD kinase, the metazoan ortholog of yeast Ctk1.

Authors: Bartlomiej Bartkowiak; Pengda Liu; Hemali P Phatnani; Nicholas J Fuda; Jeffrey J Cooper; David H Price; Karen Adelman; John T Lis; Arno L Greenleaf
Journal: Genes Dev Date: 2010-10-15 Impact factor: 11.361

Review 5. Non-canonical functions of cell cycle cyclins and cyclin-dependent kinases.

Authors: Per Hydbring; Marcos Malumbres; Piotr Sicinski
Journal: Nat Rev Mol Cell Biol Date: 2016-04-01 Impact factor: 94.444

6. Cdk-activating kinase complex is a component of human transcription factor TFIIH.

Authors: R Shiekhattar; F Mermelstein; R P Fisher; R Drapkin; B Dynlacht; H C Wessling; D O Morgan; D Reinberg
Journal: Nature Date: 1995-03-16 Impact factor: 49.962

7. The Cyclin K/Cdk12 complex maintains genomic stability via regulation of expression of DNA damage response genes.

Authors: Dalibor Blazek; Jiri Kohoutek; Koen Bartholomeeusen; Eric Johansen; Petra Hulinkova; Zeping Luo; Peter Cimermancic; Jernej Ule; B Matija Peterlin
Journal: Genes Dev Date: 2011-10-15 Impact factor: 11.361

8. Cdk12 Is A Gene-Selective RNA Polymerase II Kinase That Regulates a Subset of the Transcriptome, Including Nrf2 Target Genes.

Authors: Xuan Li; Nirmalya Chatterjee; Kerstin Spirohn; Michael Boutros; Dirk Bohmann
Journal: Sci Rep Date: 2016-02-25 Impact factor: 4.379

Review 9. Therapeutic targeting of transcriptional cyclin-dependent kinases.

Authors: Matthew D Galbraith; Heather Bender; Joaquín M Espinosa
Journal: Transcription Date: 2018-11-09

10. 3' end formation of pre-mRNA and phosphorylation of Ser2 on the RNA polymerase II CTD are reciprocally coupled in human cells.

Authors: Lee Davidson; Lisa Muniz; Steven West
Journal: Genes Dev Date: 2014-01-29 Impact factor: 11.361

9 in total

Review 1. PROTACs: great opportunities for academia and industry (an update from 2020 to 2021).

Authors: Ming He; Chaoguo Cao; Zhihao Ni; Yongbo Liu; Peilu Song; Shuang Hao; Yuna He; Xiuyun Sun; Yu Rao
Journal: Signal Transduct Target Ther Date: 2022-06-09

2. Trivalent PROTACs enhance protein degradation via combined avidity and cooperativity.

Authors: Satomi Imaide; Kristin M Riching; Nikolai Makukhin; Vesna Vetma; Claire Whitworth; Scott J Hughes; Nicole Trainor; Sarah D Mahan; Nancy Murphy; Angus D Cowan; Kwok-Ho Chan; Conner Craigon; Andrea Testa; Chiara Maniaci; Marjeta Urh; Danette L Daniels; Alessio Ciulli
Journal: Nat Chem Biol Date: 2021-10-21 Impact factor: 15.040

Discovery and resistance mechanism of a selective CDK12 degrader.

1. Three RNA polymerase II carboxyl-terminal domain kinases display distinct substrate preferences.

Review 2. Secrets of a double agent: CDK7 in cell-cycle control and transcription.

3. EWS/FLI Confers Tumor Cell Synthetic Lethality to CDK12 Inhibition in Ewing Sarcoma.

4. CDK12 is a transcription elongation-associated CTD kinase, the metazoan ortholog of yeast Ctk1.

Review 5. Non-canonical functions of cell cycle cyclins and cyclin-dependent kinases.

6. Cdk-activating kinase complex is a component of human transcription factor TFIIH.

7. The Cyclin K/Cdk12 complex maintains genomic stability via regulation of expression of DNA damage response genes.

8. Cdk12 Is A Gene-Selective RNA Polymerase II Kinase That Regulates a Subset of the Transcriptome, Including Nrf2 Target Genes.

Review 9. Therapeutic targeting of transcriptional cyclin-dependent kinases.

10. 3' end formation of pre-mRNA and phosphorylation of Ser2 on the RNA polymerase II CTD are reciprocally coupled in human cells.

Review 1. PROTACs: great opportunities for academia and industry (an update from 2020 to 2021).

2. Trivalent PROTACs enhance protein degradation via combined avidity and cooperativity.

Review 3. Transcription associated cyclin-dependent kinases as therapeutic targets for prostate cancer.

Review 4. Inhibitors, PROTACs and Molecular Glues as Diverse Therapeutic Modalities to Target Cyclin-Dependent Kinase.

Review 5. Altered pathways and targeted therapy in double hit lymphoma.

6. Profiling the Landscape of Drug Resistance Mutations in Neosubstrates to Molecular Glue Degraders.

7. CDK12 regulates co-transcriptional splicing and RNA turnover in human cells.

Review 8. Cellular senescence: a key therapeutic target in aging and diseases.

Review 9. Degraders: The Ultimate Weapon Against Amplified Driver Kinases in Cancer.