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首页> 外文期刊>Oncology Research >Detection of Necroptosis in Ligand-Mediated and Hypoxia-Induced Injury of Hepatocytes Using a Novel Optic Probe-Detecting Receptor-Interacting Protein (RIP)1/RIP3 Binding
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Detection of Necroptosis in Ligand-Mediated and Hypoxia-Induced Injury of Hepatocytes Using a Novel Optic Probe-Detecting Receptor-Interacting Protein (RIP)1/RIP3 Binding

机译:使用新型光学探针检测受体相互作用蛋白(RIP3结合

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Liver injury is often observed in various pathological conditions including posthepatectomy state and cancer chemotherapy. It occurs mainly as a consequence of the combined necrotic and apoptotic types of cell death. In order to study liver/hepatocyte injury by the necrotic type of cell death, we studied signal-regulated necrosis (necroptosis) by developing a new optic probe for detecting receptor-interacting protein kinase 1(RIP)/RIP3 binding, an essential process for necroptosis induction. In the mouse hepatocyte cell line, TIB-73 cells, TNF-alpha/cycloheximide (T/C) induced RIP1/3 binding only when caspase activity was suppressed by the caspase-specific inhibitor z-VAD-fmk (zVAD). T/C/zVAD-induced RIP1/3 binding was inhibited by necrostatin-1 (Nec-1), an allosteric inhibitor of RIP1. The reduced cell survival by T/C/zVAD was improved by Nec-1. These facts indicate that T/C induces necroptosis of hepatocytes when the apoptotic pathway is inhibited/unavailable. FasL also induced cell death, which was only partially inhibited by zVAD, indicating the possible involvement of necroptosis rather than apoptosis. FasL activated caspase 3 and, similarly, induced RIP1/3 binding when the caspases were inactivated. Interestingly. FasL-induced RIP1/3 binding was significantly suppressed by the antioxidants Trolox and N-acetyl cysteine (NAC), suggesting the involvement of reactive oxygen species (ROS) in FasL-induced necroptotic cellular processes. H2O2 . by itself. induced RIP1/3 binding that was suppressed by Nec-1. but not by zVAD. Hypoxia induced RIP1/3 binding after reoxygenation, which was suppressed by Nec-1 or by the antioxidants. Cell death induced by hypoxia/ reoxygenation (H/R) was also improved by Nec-1. Similar to H2O2 , H/R did not require caspase inhibition for RIP1/3 binding, suggesting the involvement of a caspase-independent mechanism for non-ligand-induced and/or redox-mediated necroptosis. These data indicate that ROS can induce necroptosis and mediate the FasL- and hypoxia-induced necroptosis via a molecular mechanism that differs from a conventional caspase-dependent pathway. In conclusion. necroptosis is potentially involved in liver/hepatocyte injury induced by oxidative stress and FasL in the absence of apoptosis.
机译:在各种病理病症中经常观察到肝损伤,包括治疗术治疗状态和癌症化疗。它主要是由于组合坏死和凋亡类型的细胞死亡的结果。为了通过DECROCED类型的细胞死亡研究肝脏/肝细胞损伤,我们通过开发一种用于检测受体相互作用蛋白激酶1(RIP)/ RIP3结合的新型光学探针来研究信号调节的坏死(Necroptosis),是死区诱导。在小鼠肝细胞系中,TIB-73细胞,TNF-α/环己酰亚胺(T / C)诱导RIP1 / 3只有当通过胱天蛋白酶的抑制剂Z-VAD-FMK(ZVAD)抑制了胱天蛋白酶活性时。 Necroostatin-1(NEC-1)抑制了R / C / ZVAD诱导的裂口1/3结合,RIP1的变构抑制剂。 NEC-1改善了T / C / ZVAD的细胞存活率降低。这些事实表明,当凋亡途径被抑制/不可用时,T / C诱导肝细胞的坏死。 FasL还诱导细胞死亡,该细胞死亡仅被ZVAD部分抑制,表明虐鼠可能受累而不是细胞凋亡。 FasL活化的Caspase 3和类似地,当胱天蛋白酶灭活时,诱导曲率曲折1/3结合。有趣的是。通过抗氧化剂滴油和N-乙酰半胱氨酸(NAC)显着抑制了FasL诱导的RIP1 / 3结合,表明反应性氧物种(ROS)参与FasL诱导的肮脏细胞方法。 H2O2。通过它自己。由NEC-1抑制的RIP1 / 3结合。但不是ZVAD。缺氧诱导RIP1 / 3雷诺后结合,其被NEC-1或抗氧化剂抑制。通过NEC-1还改善了由缺氧/雷诺基化(H / R)诱导的细胞死亡。与H 2 O 2类似,H / R不需要裂纹酶抑制RIP1 / 3结合,表明Caspase-ass-utys--或氧化还原介导的肮脏衰竭的涉及伴随的非配体诱导的粪便。这些数据表明,ROS可以通过与常规胱天蛋白酶依赖性途径不同的分子机制来诱导坏凋亡并介导FasL-和缺氧诱导的粪便。综上所述。肮脏的病症可能参与氧化胁迫和FasL在没有细胞凋亡的情况下诱导的肝脏/肝细胞损伤。

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