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赭曲霉毒素A的毒代动力学与毒效动力学:最新进展

Toxicokinetics and toxicodynamics of ochratoxin A, an update.

作者信息

Ringot Diana, Chango Abalo, Schneider Yves-Jacques, Larondelle Yvan

机构信息

Institut Supérieur d'Agriculture de Beauvais, Rue Pierre Waguet, BP 30313, Beauvais, Cedex 60026, France.

出版信息

Chem Biol Interact. 2006 Jan 5;159(1):18-46. doi: 10.1016/j.cbi.2005.10.106. Epub 2005 Nov 15.

Abstract

Ochratoxin A (OTA) is a mycotoxin produced by fungi of two genera: Penicillium and Aspergillus. OTA has been shown to be nephrotoxic, hepatotoxic, teratogenic and immunotoxic to several species of animals and to cause kidney and liver tumours in mice and rats. Because of differences in the physiology of animal species, wide variations are seen in the toxicokinetic patterns of absorption, distribution and elimination of the toxin. Biotransformation of OTA has not been entirely elucidated. At present, data regarding OTA metabolism are controversial. Several metabolites have been characterized in vitro and/or in vivo, whereas other metabolites remain to be characterized. Several major mechanisms have been shown as involved in the toxicity of OTA: inhibition of protein synthesis, promotion of membrane peroxidation, disruption of calcium homeostasis, inhibition of mitochondrial respiration and DNA damage. The contribution of metabolites in OTA genotoxicity and carcinogenicity is still unclear. The genotoxic status of OTA is still controversial because contradictory results were obtained in various microbial and mammalian tests, notably regarding the formation of DNA adducts. More recent studies are focused on the OTA ability to disturb cellular signalling and regulation, to modulate physiological signals and thereby to influence cells viability and proliferation. The present paper offers an update on these different issues. In addition since humans and animals are likely to be simultaneously exposed to several mycotoxins, especially through their diet, the little information available on the combined effects of OTA and other mycotoxins has also been reviewed.

摘要

赭曲霉毒素A(OTA)是由青霉属和曲霉属两种真菌产生的一种霉菌毒素。OTA已被证明对多种动物具有肾毒性、肝毒性、致畸性和免疫毒性,并可导致小鼠和大鼠发生肾和肝肿瘤。由于动物物种生理机能的差异,毒素在吸收、分布和消除的毒代动力学模式上存在很大差异。OTA的生物转化尚未完全阐明。目前,关于OTA代谢的数据存在争议。几种代谢物已在体外和/或体内得到表征,而其他代谢物仍有待表征。已证明OTA毒性涉及几种主要机制:抑制蛋白质合成、促进膜过氧化、破坏钙稳态、抑制线粒体呼吸和DNA损伤。代谢物在OTA遗传毒性和致癌性中的作用仍不清楚。OTA的遗传毒性状态仍存在争议,因为在各种微生物和哺乳动物试验中获得了相互矛盾的结果,特别是关于DNA加合物的形成。最近的研究集中在OTA干扰细胞信号传导和调节、调节生理信号从而影响细胞活力和增殖的能力上。本文提供了关于这些不同问题的最新情况。此外,由于人类和动物可能同时接触多种霉菌毒素,特别是通过饮食接触,关于OTA与其他霉菌毒素联合作用的现有信息也已得到综述。

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