Gonzalez Susana, Perez-Perez Manuel M, Hernando Eva, Serrano Manuel, Cordon-Cardo Carlos
Department of Pathology, Memorial Sloan-Kettering Cancer Center, New York, NY, USA.
Cancer Res. 2005 Mar 15;65(6):2186-92. doi: 10.1158/0008-5472.CAN-04-3047.
Similarly to p53, p73alpha and p73beta induce growth arrest and/or apoptosis in response to DNA damage or when exogenously expressed. However, how they trigger apoptosis remains unresolved. After stable transduction of either p73alpha or p73beta, a greater apoptotic response was observed for p73beta in both primary and tumor cells. Consistently, blocking ectopic and endogenous p73beta expression by specific shRNA significantly decreased apoptotic levels after DNA damage. We found that p73beta targets the apoptotic program at multiple levels: (i) facilitating caspase activation through p53-dependent signals and (ii) inducing p57KIP2, while down-regulating c-IPA1 and IEX1 through a p53-independent mechanism. p73beta-mediated apoptosis was considerably reduced after inhibition of p57(KIP2) by small interfering RNA, IEX-1 overexpression, and in mouse embryo fibroblasts derived from p57-/- mice. Data from this study offer evidence for the apoptotic activity exclusive of p73beta. In the clinical context, these results might have potential therapeutic implications, because p73beta could induce alternative apoptotic responses in tumors harboring p53 mutations.
与p53类似,p73α和p73β在DNA损伤时或外源表达时可诱导细胞生长停滞和/或凋亡。然而,它们如何触发凋亡仍未解决。在稳定转导p73α或p73β后,在原代细胞和肿瘤细胞中均观察到p73β有更强的凋亡反应。同样,通过特异性短发夹RNA阻断异位和内源性p73β表达可显著降低DNA损伤后的凋亡水平。我们发现p73β在多个水平靶向凋亡程序:(i)通过p53依赖信号促进半胱天冬酶激活,以及(ii)诱导p57KIP2,同时通过p53非依赖机制下调c-IPA1和IEX1。在用小分子干扰RNA抑制p57(KIP2)、IEX-1过表达以及在源自p57-/-小鼠的小鼠胚胎成纤维细胞中,p73β介导的凋亡显著减少。本研究的数据为p73β特有的凋亡活性提供了证据。在临床方面,这些结果可能具有潜在的治疗意义,因为p73β可在携带p53突变的肿瘤中诱导替代性凋亡反应。
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