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首页> 外文期刊>Oncogene >Differential effects of NF-|[kappa]|B on apoptosis induced by DNA-damaging agents: the type of DNA damage determines the final outcome
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Differential effects of NF-|[kappa]|B on apoptosis induced by DNA-damaging agents: the type of DNA damage determines the final outcome

机译:NF- |κ| B对DNA损伤剂诱导的细胞凋亡的差异作用:DNA损伤的类型决定了最终结果

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摘要

The transcription factor nuclear factor kappa-B (NF-B) is generally regarded as an antiapoptotic factor. Accordingly, NF-B activation inhibits death ligand-induced apoptosis. In contrast, ultraviolet light B (UVB)-induced apoptosis is not inhibited but even enhanced upon NF-B activation by interleukin-1 (IL-1). This study was performed to identify the molecular mechanisms underlying this switch of NF-B. Enhancement of UVB-induced apoptosis was always associated with increased release of tumour necrosis factor- (TNF-), which was dependent on NF-B activation. The same was observed when UVA and cisplatin were used, which like UVB induce base modifications. In contrast, apoptosis caused by DNA strand breaks was not enhanced by IL-1, indicating that the type of DNA damage is critical for switching the effect of NF-B on apoptosis. Surprisingly, activated NF-B induced TNF- mRNA expression in the presence of all DNA damage-inducing agents. However, in the presence of DNA strand breaks, there was no release of the TNF- protein, which is so crucial for enhancing apoptosis. Together, this indicates that induction of DNA damage may have a significant impact on biological effects but it is the type of DNA damage that determines the final outcome. This may have implications for the role of NF-B in carcinogenesis and for the application of NF-B inhibitors in anticancer therapy.
机译:转录因子核因子κB(NF-B)通常被认为是抗凋亡因子。因此,NF-B激活抑制死亡配体诱导的凋亡。相反,紫外线B(UVB)诱导的凋亡不会受到抑制,而白介素1(IL-1)激活NF-B时甚至会增强。进行这项研究是为了确定这种NF-B转换的分子机制。 UVB诱导的细胞凋亡增强始终与肿瘤坏死因子-(TNF-)的释放增加有关,而肿瘤坏死因子-(TNF-)的释放依赖于NF-B的激活。当使用UVA和顺铂时,也观察到了同样的情况,它们像UVB一样会诱导碱基修饰。相反,IL-1不能增强DNA链断裂引起的凋亡,这表明DNA损伤的类型对于切换NF-B对凋亡的作用至关重要。令人惊讶地,在所有DNA损伤诱导剂的存在下,活化的NF-B诱导了TNF-mRNA表达。然而,在DNA链断裂的情况下,没有释放TNF-蛋白,这对于增强细胞凋亡至关重要。总之,这表明DNA损伤的诱导可能会对生物学效应产生重大影响,但是DNA损伤的类型决定了最终结果。这可能与NF-B在致癌作用中的作用以及NF-B抑制剂在抗癌治疗中的应用有关。

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