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Treat cancers by targeting survivin: Just a dream or future reality?

机译:通过靶向生存素治疗癌症:只是梦想还是未来的现实?

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摘要

Since the discovery of survivin (BIRC5) as a cancer-related molecule by Grazia Ambrosini and Dario C. Altieri at 1997, our knowledge related to the function of this molecule has been extended from simple apoptosis inhibition to complicated, interlinked processes that involve interference of mitosis, apoptosis, autophagy, and even DNA repair recently. However, despite the growing amount of knowledge related to survivin in the last ten years, the development of survivin inhibitors or survivin-related molecular therapies is surprisingly and relatively slow as compared to other therapeutic inhibitors for cancer treatment. Here, the molecular functions of survivin and the progress of development of survivin-targeting therapies are discussed in detail. Functional differences between different survivin-specific inhibitors are discussed from both structural and biochemical point of views. This review also reveals different challenges that scientists are currently facing in the development of survivin inhibitors for clinical application. Finally, future directions for the development of survivin-targeted therapies are discussed in this review.
机译:自1997年Grazia Ambrosini和Dario C.Altieri发现Survivin(BIRC5)是一种与癌症相关的分子以来,我们对这种分子功能的认识已从简单的细胞凋亡抑制作用扩展到涉及相互干扰的复杂,相互联系的过程。最近有丝分裂,凋亡,自噬甚至DNA修复。然而,尽管在最近十年中与存活蛋白有关的知识越来越多,但是与其他用于癌症治疗的抑制剂相比,存活蛋白抑制剂或与存活蛋白相关的分子疗法的发展令人惊讶且相对缓慢。在此,详细讨论了survivin的分子功能和靶向survivin的疗法的发展进展。从结构和生化的角度讨论了不同的survivin特异性抑制剂之间的功能差异。这篇综述还揭示了科学家目前在开发用于临床应用的生存素抑制剂方面面临的不同挑战。最后,在这篇综述中讨论了以生存素为靶标的疗法的未来发展方向。

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