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使用基于生理学的药代动力学模型和体外到体内外推法解决早期生活敏感性问题。

Addressing Early Life Sensitivity Using Physiologically Based Pharmacokinetic Modeling and In Vitro to In Vivo Extrapolation.

作者信息

Yoon Miyoung, Clewell Harvey J

机构信息

The Hamner Institutes for Health Sciences.

出版信息

Toxicol Res. 2016 Jan;32(1):15-20. doi: 10.5487/TR.2016.32.1.015. Epub 2016 Jan 31.

Abstract

Physiologically based pharmacokinetic (PBPK) modeling can provide an effective way to utilize in vitro and in silico based information in modern risk assessment for children and other potentially sensitive populations. In this review, we describe the process of in vitro to in vivo extrapolation (IVIVE) to develop PBPK models for a chemical in different ages in order to predict the target tissue exposure at the age of concern in humans. We present our on-going studies on pyrethroids as a proof of concept to guide the readers through the IVIVE steps using the metabolism data collected either from age-specific liver donors or expressed enzymes in conjunction with enzyme ontogeny information to provide age-appropriate metabolism parameters in the PBPK model in the rat and human, respectively. The approach we present here is readily applicable to not just to other pyrethroids, but also to other environmental chemicals and drugs. Establishment of an in vitro and in silico-based evaluation strategy in conjunction with relevant exposure information in humans is of great importance in risk assessment for potentially vulnerable populations like early ages where the necessary information for decision making is limited.

摘要

基于生理学的药代动力学(PBPK)模型能够提供一种有效方法,在针对儿童及其他潜在敏感人群的现代风险评估中利用基于体外和计算机模拟的信息。在本综述中,我们描述了体外到体内外推(IVIVE)的过程,以针对不同年龄段的一种化学物质建立PBPK模型,从而预测人类关注年龄时的靶组织暴露情况。我们展示了正在进行的关于拟除虫菊酯的研究,作为一个概念验证,使用从特定年龄肝脏供体收集的代谢数据或表达的酶结合酶个体发生信息,分别在大鼠和人类的PBPK模型中提供适合年龄的代谢参数,引导读者了解IVIVE步骤。我们在此介绍的方法不仅适用于其他拟除虫菊酯,也适用于其他环境化学物质和药物。结合人类相关暴露信息建立基于体外和计算机模拟的评估策略,对于像早期年龄段这样决策所需信息有限的潜在脆弱人群的风险评估非常重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ea68/4780231/b19ad48f4265/tr-32-015f1.jpg

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