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Unfolded protein response to autophagy as a promising druggable target for anticancer therapy

机译:展开蛋白质反应自噬作为抗癌治疗的有前途的可用毒性目标

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The endoplasmic reticulum (ER) is responsible for protein processing. In rapidly proliferating tumor cells, the ER tends to be overloaded with unfolded and misfolded proteins due to high metabolic demand. With the limited protein-folding capacity of the ER, tumor cells often suffer from more ER stress than do normal cells. Thus, cellular stress responses to cope with ER stress, such as the unfolded protein response (UPR) and autophagy, might be more activated in cancer cells than in normal cells. The complex signaling pathways from the UPR to autophagy provide promising druggable targets; a number of UPR/autophagy-targeted anticancer agents are currently in development in preclinical and clinical studies. In this short review we will discuss the potential anticancer efficacy of modulators of cellular stress responses, especially UPR and autophagy, on the basis of their signaling pathways. In addition, the current developmental status of the UPR/autophagy-targeted agents will be discussed.
机译:内质网(ER)负责蛋白质加工。在快速增殖的肿瘤细胞中,由于高代谢需求,ER趋于用展开和错误折叠的蛋白质过载。随着ER的有限蛋白质折叠能力,肿瘤细胞通常患有比正常细胞更高的ER应力。因此,对癌细胞中的诸如展开蛋白质反应(UPR)和自噬的诸如展开蛋白质反应(UPR)和自噬的细胞应激反应可能比在正常细胞中更高。从UPR到自噬的复杂信号通路提供了有前途的可用性靶标;许多UPR /自噬有针对性的抗癌剂目前正在临床前和临床研究中开发。在这次简短的审查中,我们将在其信号通路的基础上讨论细胞应激反应,尤其是UPR和自噬的调节剂的潜在抗癌疗效。此外,将讨论UPR /自噬靶向代理的目前发育状况。

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