| Literature DB >> 29025359 |
Hana Paculová1, Juraj Kramara2, Šárka Šimečková3,4, Radek Fedr3,5, Karel Souček3,4,5, Ondřej Hylse5,6, Kamil Paruch5,6, Marek Svoboda7, Martin Mistrík2, Jiří Kohoutek1.
Abstract
A broad spectrum of tumors develop resistance to classic chemotherapy, necessitating the discovery of new therapies. One successful strategy exploits the synthetic lethality between poly(ADP-ribose) polymerase 1/2 proteins and DNA damage response genes, including BRCA1, a factor involved in homologous recombination-mediated DNA repair, and CDK12, a transcriptional kinase known to regulate the expression of DDR genes. CHK1 inhibitors have been shown to enhance the anti-cancer effect of DNA-damaging compounds. Since loss of BRCA1 increases replication stress and leads to DNA damage, we tested a hypothesis that CDK12- or BRCA1-depleted cells rely extensively on S-phase-related CHK1 functions for survival. The silencing of BRCA1 or CDK12 sensitized tumor cells to CHK1 inhibitors in vitro and in vivo. BRCA1 downregulation combined with CHK1 inhibition induced excessive amounts of DNA damage, resulting in an inability to complete the S-phase. Therefore, we suggest CHK1 inhibition as a strategy for targeting BRCA1- or CDK12-deficient tumors.Entities:
Keywords: BRCA1; CDK12; CHK1 inhibitor; DNA damage response; transcription
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Year: 2017 PMID: 29025359 DOI: 10.1177/1010428317727479
Source DB: PubMed Journal: Tumour Biol ISSN: 1010-4283