The Targeted Inhibition of Mitochondrial Hsp90 Overcomes The Apoptosis Resistance Conferred By Bcl-2

来源 :3rd Asian Conference on Environmental Mutagens & 15th Confer | 被引量 : 0次 | 上传用户:jimmy7872
下载到本地 , 更方便阅读
声明 : 本文档内容版权归属内容提供方 , 如果您对本文有版权争议 , 可与客服联系进行内容授权或下架
论文部分内容阅读
  Previous studies presented that Gamitrinibs rapidly accumulate in tumor cell mitochondria, lead cells to apoptotic pathway in tumor cells.Thus Gamitrinibs are considered a series of promising drugs for cancer.However, a cell can die in different types e.g.apoptosis, necrosis or necroptosis, and autophagic cell death.In this study we aimed to further investigate the mechanisms and modes of cell death in G-TPP-treated Hep3B and U937 cell lines.It was observed that G-TPP killed U937 cells majorly in apoptotic pathway,and Hep3B cells majorly via activating caspase-independent necrosis and/or necroptosis with in part caspase-dependant apoptosis.Simultaneously, we observed G-TPP induced compensatory autophagy in Hep3B cell lines.Overexpression Bcl-2 significantly inhibited cell death in U937 cells, but not in Hep3B cells, contrarily, increase cell sensitiveness to G-TPP.We further probed it and found Bcl-2-Beclin 1 interaction in response to G-TPP by immunoprecipitation assay.However, silencing of beclin 1 failed to block accumulation of LC3 Ⅱ in Hep3B cells.Taken together, these data reveal that G-TPP induce cell death via apoptotic pathway in U937 cells, and a combination of death pathways, including necrosis and/or necroptosis and apoptosis Otherwise, G-TPP trigger Beclin 1-independant protective autophagy in Hep3B cells.Overexpression of Bcl-2 protein may be involved in other pathways to response to G-TPP and increase cells sensitive to G-TPP in Hep3B cells.The data are important for the therapeutic exploitation of necroptosis and/or necrosis as an alternative cell death program to bypass apoptosis resistance.
其他文献
  Due to their toxicity, the increased distribution of microcystins (MCs) has become an important worldwide problem.MCs have been recognized as inhibitors of
会议
会议
会议
  Objective: To explore the effects of vinyl chloride monomer (VCM) on cell cycle and apoptosis of hepatocytes in rats.Methods: Sixty-four Sprague Dawley (SD)
会议
会议
会议
  Methyl methanesulfonate (MMS) has been shown to induce apoptosis in various cell types through p53-dependent pathways.Nevertheless, pharmacological and gene
会议