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卤代乙烯基半胱氨酸化合物的肾毒性。

Nephrotoxicity of halogenated vinyl cysteine compounds.

作者信息

Gandolfi A J, Nagle R B, Soltis J J, Plescia F H

出版信息

Res Commun Chem Pathol Pharmacol. 1981 Aug;33(2):249-61.

PMID:7302373
Abstract

S-(1,2-dichlorovinyl) cysteine (DCVC), is a potent nephrotoxin. In order to determine if other vinyl cysteine conjugates were nephrotoxic, halogenated vinyl cysteines, HVC-1 and HVC-2, were prepared from chlorotrifluoroethylene (CTFE), a fluorocarbon monomer, or chlorotifluoroethylene, a metabolite of halothane, respectively. Three days after receiving DCVC (5-10 mg/kg), CD-1 mice developed focal renal tubular necrosis. Mice treated with HVC-1 or HVC-2 (5-10 mg/kg) also developed renal necrosis by 3 days post exposure. HVC-1 was not as potent as DCVC with the necrosis limited to the pars recta. At equivalent doses HVC-2 caused less necrosis of the pars recta than HVC-1. The degree of nephrotoxicity by all three compounds exhibited a dose-response from 1-25 mg/kg. Doses greater than 25 mg/kg were often lethal within 3 days and the mice had a complete zonal necrosis of the renal cortex and a two-fold increase in kidney weight. Structural analogues, S-(chlorethyl) or S-(hydroxyethyl) cysteine, did not cause renal necrosis in mice at doses up to 200 mg/kg. These studies indicate that the enzymes reportedly responsible for converting DCVC to a nephrotoxic intermediate will also bioactivate other halogenated vinyl cysteines.

摘要

S-(1,2-二氯乙烯基)半胱氨酸(DCVC)是一种强效肾毒素。为了确定其他乙烯基半胱氨酸共轭物是否具有肾毒性,分别由氟碳单体三氟氯乙烯(CTFE)或氟烷的代谢产物三氟氯乙烯制备了卤代乙烯基半胱氨酸HVC-1和HVC-2。给予DCVC(5-10mg/kg)三天后,CD-1小鼠出现局灶性肾小管坏死。用HVC-1或HVC-2(5-10mg/kg)处理的小鼠在暴露后3天也出现了肾坏死。HVC-1的效力不如DCVC,坏死仅限于直部。在等效剂量下,HVC-2引起的直部坏死比HVC-1少。所有三种化合物的肾毒性程度在1-25mg/kg范围内呈现剂量反应关系。大于25mg/kg的剂量通常在3天内致死,小鼠肾皮质出现完全的带状坏死,肾脏重量增加两倍。结构类似物S-(氯乙基)或S-(羟乙基)半胱氨酸在高达200mg/kg的剂量下不会引起小鼠肾坏死。这些研究表明,据报道负责将DCVC转化为肾毒性中间体的酶也会使其他卤代乙烯基半胱氨酸生物活化。

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