Inhibition of Chk1 stimulates cytotoxic action of platinum-based drugs and TRAIL combination in human prostate cancer cells

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Publikace nespadá pod Fakultu sportovních studií, ale pod Přírodovědeckou fakultu. Oficiální stránka publikace je na webu muni.cz.
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KRKOŠKA Martin PARUCH Kamil ŠOŠOLÍKOVÁ Tereza VÁZQUEZ-GÓMEZ Gerardo HERŮDKOVÁ Jarmila NOVOTNÝ Jan OVESNÁ Petra SOVA Petr HYRŠLOVÁ VACULOVÁ Alena

Rok publikování 2024
Druh Článek v odborném periodiku
Časopis / Zdroj Biological Chemistry
Fakulta / Pracoviště MU

Přírodovědecká fakulta

Citace
www https://www.degruyter.com/document/doi/10.1515/hsz-2023-0111/html
Doi http://dx.doi.org/10.1515/hsz-2023-0111
Klíčová slova checkpoint kinase 1; SCH900776; cisplatin; TRAIL; cell death; prostate cancer
Popis Checkpoint kinase 1 (Chk1) plays an important role in regulation of the cell cycle, DNA damage response and cell death, and represents an attractive target in anticancer therapy. Small-molecule inhibitors of Chk1 have been intensively investigated either as single agents or in combination with various chemotherapeutic drugs and they can enhance the chemosensitivity of numerous tumor types. Here we newly demonstrate that pharmacological inhibition of Chk1 using potent and selective inhibitor SCH900776, currently profiled in phase II clinical trials, significantly enhances cytotoxic effects of the combination of platinum-based drugs (cisplatin or LA-12) and TRAIL (tumor necrosis factor-related apoptosis inducing ligand) in human prostate cancer cells. The specific role of Chk1 in the drug combination-induced cytotoxicity was confirmed by siRNA-mediated silencing of this kinase. Using RNAi-based methods we also showed the importance of Bak-dependent mitochondrial apoptotic pathway in the combined anticancer action of SCH900776, cisplatin and TRAIL. The triple drug combination-induced cytotoxicity was partially enhanced by siRNA-mediated Mcl-1 silencing. Our findings suggest that targeting Chk1 may be used as an efficient strategy for sensitization of prostate cancer cells to killing action of platinum-based chemotherapeutic drugs and TRAIL.
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