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砷与蛋白质结合的治疗及分析应用

Therapeutic and analytical applications of arsenic binding to proteins.

作者信息

Chen Beibei, Liu Qingqing, Popowich Aleksandra, Shen Shengwen, Yan Xiaowen, Zhang Qi, Li Xing-Fang, Weinfeld Michael, Cullen William R, Le X Chris

机构信息

Division of Analytical and Environmental Toxicology, Department of Laboratory Medicine and Pathology, University of Alberta, Edmonton, Canada.

出版信息

Metallomics. 2015 Jan;7(1):39-55. doi: 10.1039/c4mt00222a. Epub 2014 Oct 30.

Abstract

Arsenic binding to proteins plays a pivotal role in the health effects of arsenic. Further knowledge of arsenic binding to proteins will advance the development of bioanalytical techniques and therapeutic drugs. This review summarizes recent work on arsenic-based drugs, imaging of cellular events, capture and purification of arsenic-binding proteins, and biosensing of arsenic. Binding of arsenic to the promyelocytic leukemia fusion oncoprotein (PML-RARα) is a plausible mode of action leading to the successful treatment of acute promyelocytic leukemia (APL). Identification of other oncoproteins critical to other cancers and the development of various arsenicals and targeted delivery systems are promising approaches to the treatment of other types of cancers. Techniques for capture, purification, and identification of arsenic-binding proteins make use of specific binding between trivalent arsenicals and the thiols in proteins. Biarsenical probes, such as FlAsH-EDT2 and ReAsH-EDT2, coupled with tetracysteine tags that are genetically incorporated into the target proteins, are used for site-specific fluorescence labelling and imaging of the target proteins in living cells. These allow protein dynamics and protein-protein interactions to be studied. Arsenic affinity chromatography is useful for purification of thiol-containing proteins, and its combination with mass spectrometry provides a targeted proteomic approach for studying the interactions between arsenicals and proteins in cells. Arsenic biosensors evolved from the knowledge of arsenic resistance and arsenic binding to proteins in bacteria, and have now been developed into analytical techniques that are suitable for the detection of arsenic in the field. Examples in the four areas, arsenic-based drugs, imaging of cellular events, purification of specific proteins, and arsenic biosensors, demonstrate important therapeutic and analytical applications of arsenic protein binding.

摘要

砷与蛋白质的结合在砷对健康的影响中起着关键作用。对砷与蛋白质结合的进一步了解将推动生物分析技术和治疗药物的发展。本综述总结了近期在基于砷的药物、细胞事件成像、砷结合蛋白的捕获与纯化以及砷的生物传感方面的工作。砷与早幼粒细胞白血病融合癌蛋白(PML-RARα)的结合是导致急性早幼粒细胞白血病(APL)成功治疗的一种合理作用方式。鉴定对其他癌症至关重要的其他癌蛋白以及开发各种砷化合物和靶向递送系统是治疗其他类型癌症的有前景的方法。捕获、纯化和鉴定砷结合蛋白的技术利用了三价砷化合物与蛋白质中硫醇之间的特异性结合。双砷探针,如FlAsH-EDT2和ReAsH-EDT2,与基因掺入靶蛋白的四半胱氨酸标签偶联,用于活细胞中靶蛋白的位点特异性荧光标记和成像。这些可用于研究蛋白质动力学和蛋白质-蛋白质相互作用。砷亲和色谱法可用于纯化含硫醇的蛋白质,其与质谱联用为研究细胞中砷化合物与蛋白质之间的相互作用提供了一种靶向蛋白质组学方法。砷生物传感器源于对细菌中砷抗性和砷与蛋白质结合的认识,现已发展成为适用于现场检测砷的分析技术。基于砷的药物、细胞事件成像、特定蛋白质的纯化和砷生物传感器这四个领域的实例展示了砷与蛋白质结合在治疗和分析方面的重要应用。

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