Degradation of CCNK/CDK12 is a druggable vulnerability of colorectal cancer

Sebastian M. Dieter; Christine Siegl; Paula Codó; Mario Huerta; Anna L. Ostermann-Parucha; Erik Schulz; Martina K. Zowada; Sylvia Martin; Karin Laaber; Ali Nowrouzi; Mona Blatter; Sina Kreth; Frank Westermann; Axel Benner; Ulrike Uhrig; Kerstin Putzker; Joe Lewis; Andrea Haegebarth; Dominik Mumberg; Simon J. Holton; Joerg Weiske; Lena-Marit Toepper; U. Scheib; Gerhard Siemeister; Claudia R. Ball; Bernhard Küster; Gabriele Stoehr; Hannes Hahne; Sarah Johannes; Martin Lange; Friederike Herbst; Hanno Glimm

doi:10.1016/j.celrep.2021.109394

Degradation of CCNK/CDK12 is a druggable vulnerability of colorectal cancer

Sebastian M. Dieter(German Cancer Research Center), Christine Siegl(Merck KGaA, Darmstadt (Germany)), Paula Codó(German Cancer Research Center), Mario Huerta(German Cancer Research Center), Anna L. Ostermann-Parucha(German Cancer Research Center), Erik Schulz(Heidelberg University), Martina K. Zowada(German Cancer Research Center), Sylvia Martin(German Cancer Research Center), Karin Laaber(German Cancer Research Center), Ali Nowrouzi(Heidelberg University), Mona Blatter(Heidelberg University), Sina Kreth(Heidelberg University), Frank Westermann(Heidelberg University), Axel Benner(Heidelberg University), Ulrike Uhrig(European Molecular Biology Laboratory), Kerstin Putzker(European Molecular Biology Laboratory), Joe Lewis(European Molecular Biology Laboratory), Andrea Haegebarth(Bayer (Germany)), Dominik Mumberg(Bayer (Germany)), Simon J. Holton(Nuvisan (Germany)), Joerg Weiske(Nuvisan (Germany)), Lena-Marit Toepper(Nuvisan (Germany)), U. Scheib(Nuvisan (Germany)), Gerhard Siemeister(Nuvisan (Germany)), Claudia R. Ball(German Cancer Research Center), Bernhard Küster(Technical University of Munich), Gabriele Stoehr, Hannes Hahne, Sarah Johannes(Bayer (Germany)), Martin Lange(Nuvisan (Germany)), Friederike Herbst(German Cancer Research Center), Hanno Glimm(German Cancer Research Center)

Cell Reports

July 1, 2021

10.1016/j.celrep.2021.109394

Cited by 89Open Access

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Abstract

Novel treatment options for metastatic colorectal cancer (CRC) are urgently needed to improve patient outcome. Here, we screen a library of non-characterized small molecules against a heterogeneous collection of patient-derived CRC spheroids. By prioritizing compounds with inhibitory activity in a subset of-but not all-spheroid cultures, NCT02 is identified as a candidate with minimal risk of non-specific toxicity. Mechanistically, we show that NCT02 acts as molecular glue that induces ubiquitination of cyclin K (CCNK) and proteasomal degradation of CCNK and its complex partner CDK12. Knockout of CCNK or CDK12 decreases proliferation of CRC cells in vitro and tumor growth in vivo. Interestingly, sensitivity to pharmacological CCNK/CDK12 degradation is associated with TP53 deficiency and consensus molecular subtype 4 in vitro and in patient-derived xenografts. We thus demonstrate the efficacy of targeted CCNK/CDK12 degradation for a CRC subset, highlighting the potential of drug-induced proteolysis for difficult-to-treat types of cancer.

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