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多异种生物抗性作为水生生物的一种细胞防御机制。

Multixenobiotic resistance as a cellular defense mechanism in aquatic organisms.

作者信息

Bard SM

机构信息

Biology Department, Mail Stop #32, Woods Hole Oceanographic Institution, Woods Hole, MA, USA

出版信息

Aquat Toxicol. 2000 Apr 1;48(4):357-389. doi: 10.1016/s0166-445x(00)00088-6.

Abstract

Multixenobiotic resistance in aquatic organisms exposed to natural toxins or anthropogenic contaminants is a phenomenon analogous to multidrug resistance in mammalian tumor cell lines tolerant of anti-cancer drugs. Multidrug resistance is commonly due to the elevated expression of transmembrane P-glycoproteins (P-gp) which actively transport a wide variety of structurally and functionally diverse compounds. The purpose of this review is to place aquatic ecotoxicological data in context of the larger multidrug resistance field of study. Information on P-glycoproteins structure, mechanism of transport, and substrate specificity gained through traditional mammalian and cell culture models is examined in conjunction with recent work on aquatic species exposed to xenobiotics both in the field and in the laboratory. The physiological function of P-glycoproteins is explored through studies of gene knockout models and expression patterns in normal tissues and tumors. The effect of xenobiotic exposures on P-gp activity and protein titer is examined in wild and captive populations of aquatic invertebrates and vertebrates. Substrate overlap and evidence of co-expression of phase I detoxification enzymes (e.g. cytochromes P450) and P-gp are presented. The role of P-gp chemosensitizers as environmental pollutants and the ecotoxicological consequences of P-gp inhibition are highlighted. The overwhelming evidence suggests that P-glycoproteins provide aquatic organisms with resistance to a wide range of natural and anthropogenic toxins.

摘要

暴露于天然毒素或人为污染物的水生生物中的多异种生物抗性,是一种类似于哺乳动物肿瘤细胞系中对抗癌药物耐受的多药耐药性的现象。多药耐药性通常是由于跨膜P-糖蛋白(P-gp)表达升高所致,P-糖蛋白可主动转运多种结构和功能各异的化合物。本综述的目的是将水生生态毒理学数据置于更广泛的多药耐药性研究领域的背景下。结合近期在野外和实验室中对暴露于异种生物的水生物种的研究,考察通过传统哺乳动物和细胞培养模型获得的有关P-糖蛋白结构、转运机制和底物特异性的信息。通过对基因敲除模型以及正常组织和肿瘤中的表达模式的研究,探索P-糖蛋白的生理功能。在水生无脊椎动物和脊椎动物的野生和圈养种群中,考察异种生物暴露对P-gp活性和蛋白滴度的影响。介绍底物重叠以及I相解毒酶(如细胞色素P450)和P-gp共表达的证据。强调P-gp化学增敏剂作为环境污染物的作用以及P-gp抑制的生态毒理学后果。压倒性的证据表明,P-糖蛋白为水生生物提供了对多种天然和人为毒素的抗性。

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