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Autophagy genes as tumor suppressors

机译:自噬基因作为肿瘤抑制因子

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Autophagy, originally described as a universal lysosome-dependent bulk degradation of cytoplasmic components upon nutrient deprivation, has since been shown to influence diverse aspects of homeostasis and is implicated in a wide variety of pathological conditions, including cancer. The list of autophagy-related (Atg) genes associated with the initiation and progression of human cancer as well as with responses to cancer therapy continues to grow as these genes are being discovered. However, whether Atg genes work through their expected mechanisms of autophagy regulation and/or through as-yet-undefined functions in the development of cancer remains to be further clarified. Here we review recent advances in the knowledge of the molecular basis of autophagy genes and their biological outputs during tumor development. A better understanding of the mechanistic link between cellular autophagy and tumor growth control may ultimately better human cancer treatments.
机译:自噬最初被描述为营养物剥夺后普遍溶酶体依赖性的细胞质组分整体降解,自噬已被证明可影响体内稳态的各个方面,并涉及多种病理状况,包括癌症。随着人类基因的发现,与人类癌症的发生和发展以及对癌症治疗的反应相关的自噬相关(Atg)基因的清单不断增加。然而,Atg基因是否通过其预期的自噬调节机制和/或通过尚未定义的功能发挥作用来发展癌症,仍有待进一步阐明。在这里,我们回顾自噬基因的分子基础及其在肿瘤发展过程中的生物学输出知识的最新进展。更好地了解细胞自噬与肿瘤生长控制之间的机械联系可能最终会更好地治疗人类癌症。

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