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Resistance to Arsenic- and Antimony-Based Drugs

机译:对基于砷和锑的药物的耐药性

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摘要

Organic arsenicals were the first antimicrobial agents specifically synthesized for the treatment of infectious diseases such as syphilis and sleeping sickness. For the treatment of diseases caused by trypanosomatid parasites, organic derivatives of arsenic and the related metalloid antimony are still the drugs of choice. Arsenic trioxide, As203, has been used for a long time in traditional Chinese medicines for treatment of various diseases, and it has recently been shown to be clinically active in acute promyelocytic leukemias. Resistance to metalloid salts is found in bacteria, fungi, parasites and animals. In some organisms, resistance involves overproduction of intracellular thiols. In many cases, resistance to arsenic salts is the result of removal of the metalloid from the cytosol usually by extrusion from the cell. In eukaryotes resistance to arsenic and antimony is conferred by membrane transport proteins of the MRP family. The human MRP1, a member of this family, is frequently amplified in cancer cells and it is well-documented that MRPl-overexpressing cells poorly accumulate arsenic and antimony because of enhanced cellular effiux which depends on the presence of GSH.
机译:有机砷是专门合成用于治疗梅毒和昏睡病等传染病的首批抗菌剂。对于由锥虫病寄生虫引起的疾病的治疗,砷的有机衍生物和相关的准金属锑仍然是首选药物。三氧化二砷As203在传统中药中已长期使用,可用于治疗多种疾病,最近已证明在急性早幼粒细胞白血病中具有临床活性。在细菌,真菌,寄生虫和动物中发现了对准金属盐的抗性。在某些生物中,耐药性涉及细胞内硫醇的过量生产。在许多情况下,对砷盐的抗性是通常通过从细胞中挤出从细胞质中去除准金属的结果。在真核生物中,MRP家族的膜转运蛋白赋予了对砷和锑的抗性。作为该家族成员的人MRP1经常在癌细胞中扩增,并且有据可查的是,过量表达MRP1的细胞由于依赖于GSH的增强的细胞效率而难以积累砷和锑。

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