Lövborg Henrik, Wojciechowski Jacek, Larsson Rolf, Wesierska-Gadek Józefa
Department of Clinical Pharmacology, Uppsala University Hospital, Uppsala, Sweden.
Cancer Res. 2002 Aug 1;62(15):4206-11.
We observed stronger cytotoxic effect of CHS 828 on poly(ADP-ribose) polymerase-1(PARP-1) knock-out cells as compared with the normal counterpart. The proliferation of PARP-1 -/- cells was inhibited by a drug concentration approximately 3-fold lower than that in the normal cells. The monitoring of p53 levels revealed that CHS 828 induced p53 response in a dose-dependent manner in only normal cells. The drug, however, failed to activate the p53 protein in PARP-1-deficient cells even after combined treatment with multidrug-resistant modulators. These results show that the PARP-1 inactivation sensitizes cells to the novel anticancer drug CHS 828 and that the drug is able to activate different cellular pathways depending on PARP-1 status.
我们观察到,与正常细胞相比,CHS 828对聚(ADP-核糖)聚合酶-1(PARP-1)基因敲除细胞具有更强的细胞毒性作用。PARP-1基因敲除细胞增殖受到抑制时的药物浓度,比正常细胞低约3倍。对p53水平的监测显示,CHS 828仅在正常细胞中以剂量依赖性方式诱导p53反应。然而,即使在与多药耐药调节剂联合治疗后,该药物仍无法在PARP-1缺陷细胞中激活p53蛋白。这些结果表明,PARP-1失活使细胞对新型抗癌药物CHS 828敏感,并且该药物能够根据PARP-1状态激活不同的细胞途径。
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