评估内分泌干扰物的表观基因组终点的体外和体内测试方法。

ALTEX Pub Date : 2013-01-01 DOI:10.14573/altex.2013.4.445
John M Greally, Miriam N Jacobs
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引用次数: 60

摘要

表观遗传调节是关键发育过程的基础,并有助于确定成人表型。由于在敏感发育时期暴露于环境损害,表型的改变是通过受影响组织中表观遗传程序的改变来介导的。最初是为经济合作与发展组织(OECD)准备的,这篇详细的综述评估了化学物质诱导的表观遗传修饰在敏感暴露窗口期间对内分泌信号通路的潜在作用,作为内分泌干扰的一种机制,同时研究了评估这种干扰的潜在方法。在与信号通路相关的假定不良结果通路中,确定了潜在的破坏目标,并进行了有希望在筛选和测试程序中评估目标的分析,以便在可能的情况下使用体外方法,并且仅在体外方法不可用的情况下使用动物实验。监测这些表观遗传标记对毒物暴露的反应可能会在未来为预测不良后果提供一个有价值的工具,但仍然需要一个更可靠的基础来推荐测试指南。尽管有证据表明表观基因组失调可能介导暴露于内分泌干扰物的影响,但尚不确定这些变化是否真的能预测不良后果。在经合组织跨代测定中观察到的不良影响可用于为未来专门设计用于研究作用的表观遗传机制的试验提供信息。后续研究应包括表观遗传学和基因组成分,以区分潜在补偿机制的贡献。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
In vitro and in vivo testing methods of epigenomic endpoints for evaluating endocrine disruptors.

Epigenetic modulations underlie critical developmental processes and contribute to determining adult phenotype. Alterations to the phenotype, due to exposure to environmental insults during sensitive periods of development, are mediated through alterations in epigenetic programming in affected tissues. Originally prepared for the Organisation of Economic Cooperation and Development (OECD), this detailed review evaluates the potential role of chemical-induced epigenetic modifications to endocrine signaling pathways during sensitive windows of exposure as a mechanism of endocrine disruption, along with the examination of potential methods for assessing such disruption. Potential targets of disruption along putative adverse outcome pathways associated with the signaling pathways are identified, along with assays that show promise in evaluating the target in a screening and testing program such that in vitro methods are used where possible, and animal experiments only where in vitro methods are not available. Monitoring such epigenetic marks in response to toxicant exposure may in future provide a valuable tool for predicting adverse outcomes, but a more robust basis for Test Guideline recommendations is still needed. Although there is evidence to suggest that epigenomic dysregulation might mediate effects of exposures to endocrine disruptors, it is uncertain as to whether these changes are truly predictive of adverse outcome(s). Adverse effects observed in the OECD transgenerational assays could be used to inform future tests specifically designed to investigate the epigenetic mechanism of action. Follow-up studies should include both an epigenetic as well as a genomic component to differentiate between the contributions of potentially compensatory mechanisms.

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