Department of Environmental Medicine, New York University School of Medicine, 341 East 25th Street, New York, NY 10100, United States of America.
Toxicol Appl Pharmacol. 2019 Jul 15;375:1-4. doi: 10.1016/j.taap.2019.05.006. Epub 2019 May 8.
Arsenic contamination impacts hundreds of millions of people in the world. Arsenic is a well-established human carcinogen and has been shown to cause skin, lung, bladder, liver, prostate and kidney cancers, in humans. Mechanisms that underlie arsenic-mediated carcinogenesis, including epigenetic alterations, remain largely unknown. Human exposure to Arsenic is reviewed, and the mechanisms of its acute and chronic toxicity and mechanisms of its carcinogenesis in humans are discussed. Arsenic is one of the few metals that is metabolized in vivo, and Arsenic methylation and how this results in a shorter half-life in vivo are discussed. A review of recent findings that Arsenic causes loss in the cellular levels of Stem Loop Binding Protein (SLBP) resulting in polyadenylation of canonical histones (H3.1) as a default, increasing levels of H3.1 protein outside of S-Phase. Malignant cell transformation is induced by knockdown of SLBP and by overexpression of polyadenylated H3.1. Arsenic induced polyadenylation of H3.1 causes enhanced levels of H3.1 protein displacing H3.3 protein from its cellular binding sites, since the two proteins differ by only 5 amino acids. Knockdown of H3.3 alone can induce carcinogenesis, and therefore displacement of functional H3.3 protein by increased H3.1 protein, is likely a mechanism of arsenic carcinogenesis.
砷污染影响着全球数亿人。砷是一种已被证实的人类致癌物质,已被证明会导致人类皮肤癌、肺癌、膀胱癌、肝癌、前列腺癌和肾癌。砷介导的致癌作用的机制,包括表观遗传改变,在很大程度上仍然未知。本文综述了人类接触砷的情况,并讨论了其急性和慢性毒性的机制以及在人类中致癌的机制。砷是少数几种在体内代谢的金属之一,讨论了砷的甲基化及其如何导致体内半衰期缩短。最近的研究发现,砷会导致细胞内茎环结合蛋白 (SLBP) 的水平降低,从而导致典型组蛋白 (H3.1) 的多聚腺苷酸化作为默认,增加 H3.1 蛋白在 S 期之外的水平。恶性细胞转化是通过 SLBP 的敲低和多聚腺苷酸化 H3.1 的过表达诱导的。砷诱导的 H3.1 多聚腺苷酸化导致 H3.1 蛋白水平升高,从而将 H3.3 蛋白从其细胞结合位点置换,因为这两种蛋白质仅相差 5 个氨基酸。单独敲低 H3.3 本身就可以诱导致癌,因此增加的 H3.1 蛋白取代功能性 H3.3 蛋白,可能是砷致癌的机制之一。
