Noxa的诱导使表达Mcl-1的人结肠癌细胞对小分子Bcl-2/Bcl-xL抑制剂ABT-737敏感。
Induction of Noxa sensitizes human colorectal cancer cells expressing Mcl-1 to the small-molecule Bcl-2/Bcl-xL inhibitor, ABT-737.
作者信息
Okumura Kenji, Huang Shengbing, Sinicrope Frank A
机构信息
Miles and Shirley Fiterman Center for Digestive Diseases and Division of Oncology, Mayo Clinic, Rochester, Minnesota 55905, USA.
出版信息
Clin Cancer Res. 2008 Dec 15;14(24):8132-42. doi: 10.1158/1078-0432.CCR-08-1665.
PURPOSE
The intrinsic drug resistance of colorectal cancers is related in part to overexpression of prosurvival Bcl-2 family proteins. We determined the effects of ABT-737, a small-molecule inhibitor of Bcl-2/Bcl-xL but not Mcl-1, on apoptosis induction alone and in combination with CPT-11 and explored mechanisms underlying their cooperativity.
EXPERIMENTAL DESIGN
Human colorectal carcinoma cell lines (HCT116 wild-type and Bax(-/-), HT-29, and RKO) were incubated with ABT-737 alone and combined with CPT-11 or bortezomib, and cell viability, caspase cleavage, and Annexin V labeling were measured. In drug-treated cell lines, protein-protein interactions were analyzed by immunoprecipitation. Lentiviral short hairpin RNA was used to knockdown Noxa expression.
RESULTS
ABT-737 induced apoptosis in a dose-dependent manner and its coadministration with the topoisomerase I inhibitor, CPT-11, resulted in a synergistic cytotoxic effect. Apoptosis induction by the drug combination was associated with enhanced caspase-8, caspase-9, and caspase-3 activation and poly(ADP-ribose) polymerase cleavage that were completely abrogated in Bax knockout cells. ABT-737 unsequestered the BH3-only protein Bim from its complex with Bcl-xL or Bcl-2 and disrupted the interaction of Bcl-xL with Bak. CPT-11 treatment up-regulated Noxa expression, as did bortezomib, and enhanced Noxa/Mcl-1 complexes. CPT-11 also disrupted the Mcl-1/Bak interaction. Knockdown of Noxa using short hairpin RNA lentiviral constructs was shown to significantly attenuate the cytotoxic effect of CPT-11 or bortezomib combined with ABT-737 and inhibited caspase-3 cleavage.
CONCLUSIONS
Induction of Noxa by CPT-11 or bortezomib can sensitize colorectal cancer cells expressing Mcl-1 to ABT-737. Up-regulation of Noxa may therefore represent an important strategy to enhance the therapeutic efficacy of ABT-737 against colorectal cancer and other solid tumors.
目的
结直肠癌的内在耐药性部分与促生存Bcl-2家族蛋白的过表达有关。我们确定了ABT-737(一种Bcl-2/Bcl-xL而非Mcl-1的小分子抑制剂)单独及与CPT-11联合使用对诱导凋亡的影响,并探讨了它们协同作用的潜在机制。
实验设计
将人结肠癌细胞系(HCT116野生型和Bax基因敲除型、HT-29和RKO)分别单独用ABT-737处理,或与CPT-11或硼替佐米联合处理,然后检测细胞活力、半胱天冬酶裂解情况以及膜联蛋白V标记情况。在药物处理的细胞系中,通过免疫沉淀分析蛋白质-蛋白质相互作用。使用慢病毒短发夹RNA敲低Noxa表达。
结果
ABT-737以剂量依赖方式诱导凋亡,其与拓扑异构酶I抑制剂CPT-11联合给药产生协同细胞毒性作用。药物组合诱导的凋亡与半胱天冬酶-8、半胱天冬酶-9和半胱天冬酶-3激活增强以及聚(ADP-核糖)聚合酶裂解有关,而在Bax基因敲除细胞中这些作用完全被消除。ABT-737使仅含BH3结构域的蛋白Bim从其与Bcl-xL或Bcl-2的复合物中释放出来,并破坏了Bcl-xL与Bak的相互作用。CPT-11处理上调了Noxa表达,硼替佐米也有此作用,且增强了Noxa/Mcl-1复合物的形成。CPT-11还破坏了Mcl-1/Bak的相互作用。使用短发夹RNA慢病毒构建体敲低Noxa可显著减弱CPT-11或硼替佐米与ABT-737联合使用的细胞毒性作用,并抑制半胱天冬酶-3裂解。
结论
CPT-11或硼替佐米诱导Noxa表达可使表达Mcl-1的结肠癌细胞对ABT-737敏感。因此,上调Noxa可能是增强ABT-737对结直肠癌和其他实体瘤治疗效果的重要策略。
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