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PI3K/Akt/mTOR Signaling Pathway and the Biphasic Effect of Arsenic in Carcinogenesis

机译:PI3K / Akt / mTOR信号通路与砷在癌变中的双相作用

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摘要

Arsenic is a naturally occurring, ubiquitous metalloid found in the Earth’s crust. In its inorganic form, arsenic is highly toxic and carcinogenic and is widely found across the globe and throughout the environment. As an International Agency for Research on Cancer–defined class 1 human carcinogen, arsenic can cause multiple human cancers, including liver, lung, urinary bladder, skin, kidney, and prostate. Mechanisms of arsenic-induced carcinogenesis remain elusive, and this review focuses specifically on the role of the PI3K/AKT/mTOR pathway in promoting cancer development. In addition to exerting potent carcinogenic responses, arsenic is also known for its therapeutic effects against acute promyelocytic leukemia. Current literature suggests that arsenic can achieve both therapeutic as well as carcinogenic effects, and this review serves to examine the paradoxical effects of arsenic, specifically through the PI3K/AKT/mTOR pathway. Furthermore, a comprehensive review of current literature reveals an imperative need for future studies to establish and pinpoint the exact conditions for which arsenic can, and through what mechanisms it is able to, differentially regulate the PI3K/AKT/mTOR pathway to maximize the therapeutic and minimize the carcinogenic properties of arsenic.
机译:砷是在地壳中发现的自然存在的无处不在的准金属。砷以其无机形式具有剧毒和致癌性,在全球和整个环境中都广泛发现。作为国际癌症研究机构定义的第1类人类致癌物,砷可引起多种人类癌症,包括肝,肺,膀胱,皮肤,肾脏和前列腺癌。砷诱导的癌变的机制仍然难以捉摸,并且本综述特别侧重于PI3K / AKT / mTOR途径在促进癌症发展中的作用。除了发挥有效的致癌作用外,砷还以其对急性早幼粒细胞白血病的治疗作用而闻名。当前的文献表明,砷可以同时达到治疗和致癌作用,本综述旨在研究砷的矛盾作用,特别是通过PI3K / AKT / mTOR途径。此外,对现有文献的全面回顾显示,迫切需要进行进一步的研究,以建立和查明砷可以通过其精确定位的条件,以及通过何种机制来差异调节PI3K / AKT / mTOR途径,从而最大程度地发挥治疗作用。尽量减少砷的致癌特性。

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