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赭曲霉毒素A和B的物种、性别及细胞类型特异性效应。

Species-, sex-, and cell type-specific effects of ochratoxin A and B.

作者信息

O'Brien E, Heussner A H, Dietrich D R

机构信息

Environmental Toxicology, University of Konstanz, Jacob-Burckhardtstr. 25, PO Box 5560 X918, D-78457, Konstanz, Germany.

出版信息

Toxicol Sci. 2001 Oct;63(2):256-64. doi: 10.1093/toxsci/63.2.256.

Abstract

The ubiquitous mycotoxin ochratoxin A (OTA) is associated with the development of urothelial tumors and nephropathies in laboratory animals and in humans with stark species and sex differences with respect to susceptibility in disease development. The mechanism of action remains unknown. OTA-mediated disruptions in normal cell-cycle control could be a major constituent of the mechanisms underlying both its carcinogenic and nephropathy-inducing activities. Assessment of OTA's toxic effects (sum of antiproliferative, apoptotic, and necrotic effects) in rat and porcine continuous cell lines and in primary cells from humans and pigs of both sexes, have displayed a similar sex- and species-sensitivity rank order to that observed in previous in vivo experiments. Furthermore, these toxic effects were observed at nM concentrations in the presence of serum in vitro, thus closely mimicking the in vivo situation. These effects were reversible in all cell types except in human primary epithelial cells of both sexes and did not appear to be primarily dependent on the amount of OTA taken up. Indeed, fibroblasts (NRK-49F) were insensitive to OTA-mediated cell cycle inhibition in spite of accumulating comparable amounts of OTA. The results presented here support the continued use of primary renal epithelial cells for the investigation of the mechanism of OTA-induced carcinogenesis and nephropathy and provide an as-yet preliminary data set that supports the existence of a causal relationship between OTA exposure and human nephropathy.

摘要

普遍存在的霉菌毒素赭曲霉毒素A(OTA)与实验动物和人类的尿路上皮肿瘤及肾病的发生有关,在疾病发生的易感性方面存在明显的物种和性别差异。其作用机制尚不清楚。OTA介导的正常细胞周期控制破坏可能是其致癌和致肾病活性潜在机制的主要组成部分。对大鼠和猪的连续细胞系以及来自人类和猪两性的原代细胞中OTA的毒性作用(抗增殖、凋亡和坏死作用的总和)评估显示,其性别和物种敏感性排序与先前体内实验中观察到的相似。此外,在体外血清存在的情况下,在纳摩尔浓度下就观察到了这些毒性作用,从而紧密模拟了体内情况。除了人类两性的原代上皮细胞外,这些作用在所有细胞类型中都是可逆的,并且似乎并不主要依赖于摄取的OTA量。实际上,成纤维细胞(NRK-49F)尽管积累了相当数量的OTA,但对OTA介导的细胞周期抑制不敏感。本文给出的结果支持继续使用原代肾上皮细胞来研究OTA诱导的致癌作用和肾病的机制,并提供了一个初步数据集,支持OTA暴露与人类肾病之间存在因果关系。

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