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肾上腺毒理学:一种评估肾上腺皮质功能毒性和类固醇生成的策略。

Adrenal toxicology: a strategy for assessment of functional toxicity to the adrenal cortex and steroidogenesis.

作者信息

Harvey Philip W, Everett David J, Springall Christopher J

机构信息

Covance Laboratories UK Ltd, Toxicology Department, Otley Road, Harrogate, North Yorkshire, UK HG3 1PY.

出版信息

J Appl Toxicol. 2007 Mar-Apr;27(2):103-15. doi: 10.1002/jat.1221.

Abstract

The adrenal is the most common toxicological target organ in the endocrine system in vivo and yet it is neglected in regulatory endocrine disruption screening and testing. There has been a recent marked increase in interest in adrenal toxicity, but there are no standardised approaches for assessment. Consequently, a strategy is proposed to evaluate adrenocortical toxicity. Human adrenal conditions are reviewed and adrenocortical suppression, known to have been iatrogenically induced leading to Addisonian crisis and death, is identified as the toxicological hazard of most concern. The consequences of inhibition of key steroidogenic enzymes and the possible toxicological modulation of other adrenal conditions are also highlighted. The proposed strategy involves an in vivo rodent adrenal competency test based on ACTH challenge to specifically examine adrenocortical suppression. The H295R human adrenocortical carcinoma cell line is also proposed to identify molecular targets, and is useful for measuring steroids, enzymes or gene expression. Hypothalamo-pituitary-adrenal endocrinology relevant to rodent and human toxicology is reviewed (with an emphasis on multi-endocrine axis effects on the adrenal and also how the adrenal affects a variety of other hormones) and the endocrinology of the H295R cell line is also described. Chemicals known to induce adrenocortical toxicity are reviewed and over 60 examples of compounds and their confirmed steroidogenic targets are presented, with much of this work published very recently using H295R cell systems. In proposing a strategy for adrenocortical toxicity assessment, the outlined techniques will provide hazard assessment data but it will be regulatory agencies that must consider the significance of such data in risk extrapolation models. The cases of etomindate and aminoglutethimide induced adrenal suppression are clearly documented examples of iatrogenic adrenal toxicity in humans. Environmentally, sentinel species, such as fish, have also shown evidence of adrenal endocrine disruption attributed to exposure to chemicals. The extent of human sub-clinical adrenal effects from environmental chemical exposures is unknown, and the extent to which environmental chemicals may act as a contributory factor to human adrenal conditions following chronic low-level exposures will remain unknown unless purposefully studied.

摘要

肾上腺是体内内分泌系统中最常见的毒理学靶器官,但在监管内分泌干扰物筛选和测试中却被忽视。最近对肾上腺毒性的关注显著增加,但尚无标准化的评估方法。因此,本文提出了一种评估肾上腺皮质毒性的策略。回顾了人类肾上腺状况,并确定医源性诱发导致艾迪生病危象和死亡的肾上腺皮质抑制是最值得关注的毒理学危害。还强调了抑制关键类固醇生成酶的后果以及其他肾上腺状况可能的毒理学调节作用。所提出的策略包括基于促肾上腺皮质激素(ACTH)激发的体内啮齿动物肾上腺功能测试,以专门检查肾上腺皮质抑制。还建议使用H295R人肾上腺皮质癌细胞系来识别分子靶点,并且该细胞系可用于测量类固醇、酶或基因表达。回顾了与啮齿动物和人类毒理学相关的下丘脑-垂体-肾上腺内分泌学(重点是多内分泌轴对肾上腺的影响以及肾上腺如何影响多种其他激素),并描述了H295R细胞系的内分泌学。对已知可诱导肾上腺皮质毒性的化学物质进行了综述,并列出了60多种化合物及其已确认的类固醇生成靶点的实例,其中许多工作是最近使用H295R细胞系统发表的。在提出肾上腺皮质毒性评估策略时,所概述的技术将提供危害评估数据,但必须由监管机构在风险外推模型中考虑此类数据的重要性。依托咪酯和氨鲁米特诱导肾上腺抑制的案例是人类医源性肾上腺毒性的明确记录实例。在环境方面,哨兵物种,如鱼类,也已显示出因接触化学物质而导致肾上腺内分泌干扰的证据。环境化学物质暴露对人类亚临床肾上腺影响的程度尚不清楚,除非有针对性地进行研究,否则在长期低水平暴露后环境化学物质可能成为人类肾上腺状况促成因素的程度仍将未知。

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