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首页> 外文期刊>Toxicology and Applied Pharmacology >Organic anion transporter (Slc22a) family members as mediators of toxicity.
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Organic anion transporter (Slc22a) family members as mediators of toxicity.

机译:有机阴离子转运蛋白(Slc22a)家族成员是毒性的介质。

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摘要

Exposure of the body to toxic organic anions is unavoidable and occurs from both intentional and unintentional sources. Many hormones, neurotransmitters, and waste products of cellular metabolism, or their metabolites, are organic anions. The same is true for a wide variety of medications, herbicides, pesticides, plant and animal toxins, and industrial chemicals and solvents. Rapid and efficient elimination of these substances is often the body's best defense for limiting both systemic exposure and the duration of their pharmacological or toxicological effects. For organic anions, active transepithelial transport across the renal proximal tubule followed by elimination via the urine is a major pathway in this detoxification process. Accordingly, a large number of organic anion transport proteins belonging to several different gene families have been identified and found to be expressed in the proximal nephron. The function of these transporters, in combination with the high volume of renal blood flow, predisposes the kidney to increased toxic susceptibility. Understanding how the kidney mediates the transport of organic anions is integral to achieving desired therapeutic outcomes in response to drug interactions and chemical exposures, to understanding the progression of some disease states, and to predicting the influence of genetic variation upon these processes. This review will focus on the organic anion transporter (OAT) family and discuss the known members, their mechanisms of action, subcellular localization, and current evidence implicating their function as a determinant of the toxicity of certain endogenous and xenobiotic agents.
机译:人体不可避免地暴露于有毒的有机阴离子中,并且是有意和无意的。许多激素,神经递质和细胞代谢的废物或其代谢产物都是有机阴离子。各种药物,除草剂,杀虫剂,动植物毒素以及工业化学品和溶剂也是如此。快速有效地消除这些物质通常是限制全身暴露及其药理或毒理作用持续时间的最佳方法。对于有机阴离子,在整个排毒过程中,跨肾近端小管的主动跨上皮运输,然后通过尿液清除是主要途径。因此,已经鉴定出属于几种不同基因家族的大量有机阴离子转运蛋白,并发现其在近端肾单位中表达。这些转运蛋白的功能与大量肾脏血流相结合,使肾脏更容易产生毒性。了解肾脏如何介导有机阴离子的运输,对于实现对药物相互作用和化学暴露的预期治疗效果,了解某些疾病状态的进展以及预测遗传变异对这些过程的影响是不可或缺的。本文将重点介绍有机阴离子转运蛋白(OAT)家族,并讨论已知成员,其作用机理,亚细胞定位以及目前的证据,这些证据暗示它们可作为确定某些内源性和异源性药物毒性的功能。

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