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DOI10.1289/EHP1655
Evaluation and Optimization of Pharmacokinetic Models for in Vitro to in Vivo Extrapolation of Estrogenic Activity for Environmental Chemicals
Casey, Warren M.1; Chang, Xiaoqing2; Allen, David G.2; Ceger, Patricia C.2; Choksi, Neepa Y.2; Hsieh, Jui-Hua4; Wetmore, Barbara A.3,5; Ferguson, Stephen S.1; DeVito, Michael J.1; Sprankle, Catherine S.2; Kleinstreuer, Nicole C.1
2018-09-01
发表期刊ENVIRONMENTAL HEALTH PERSPECTIVES
ISSN0091-6765
EISSN1552-9924
出版年2018
卷号126期号:9
文章类型Article
语种英语
国家USA
英文摘要

BACKGROUND: To effectively incorporate in vitro data into regulatory use, confidence must be established in the quantitative extrapolation of in vitro activity to relevant end points in animals or humans.


OBJECTIVE: Our goal was to evaluate and optimize in vitro to in vivo extrapolation (IVIVE) approaches using in vitro estrogen receptor to predict estrogenic effects measured in rodent uterotrophic studies.


METHODS: We evaluated three phammcokinetic (PK) models with varying complexities to extrapolate in vitro to in vivo dosimetry for a group of 29 ER agonists, using data from validated in vitro [U.S. Environmental Protection Agency (U.S. EPA) ToxCast (TM) ER model] and in vivo (uterotrophic) methods. In vitro activity values were adjusted using mass-balance equations to estimate intracellular exposure via an enrichment factor (EF), and steady-state model calculations were adjusted using fraction of unbound chemical in the plasma (f(n)) to approximate bioavailahility. Accuracy of each model-adjustment combination was assessed by comparing model predictions with lowest effect levels (LEL5) from guideline uterotrophic studies.


RESULTS: We found little difference in model predictive performance based on complexity or route-specific modifications. Simple adjustments, applied to account for in vitro intracellular exposure (EF) or chemical bioavailability (f(u)), resulted in significant improvements in the predictive performance of all models.


CONCLUSION: Computational IVIVE approaches accurately estimate chemical exposure levels that elicit positive responses in the rodent uterotrophic bioassay. The simplest model had the best overall performance for predicting both oral (PPKEF) and injection (PPK_f(u)) LELs from guideline uterotrophic studies, is freely available, and can be parameterized entirely using freely available in silico tools.


领域资源环境
收录类别SCI-E
WOS记录号WOS:000449118800001
WOS关键词PLASMA-PROTEIN BINDING ; BISPHENOL-A ; ANDROGEN 17-ALPHA-METHYLTESTOSTERONE ; SERUM CONCENTRATIONS ; TOXCAST PROGRAM ; EXPOSURE ; BIOACTIVITY ; GENISTEIN ; ASSAYS ; DRUG
WOS类目Environmental Sciences ; Public, Environmental & Occupational Health ; Toxicology
WOS研究方向Environmental Sciences & Ecology ; Public, Environmental & Occupational Health ; Toxicology
引用统计
文献类型期刊论文
条目标识符http://119.78.100.173/C666/handle/2XK7JSWQ/24195
专题资源环境科学
作者单位1.NIEHS, Natl Toxicol Program Div, NIH, POB 12233, Res Triangle Pk, NC 27709 USA;
2.Integrated Lab Syst Inc, Morrisville, NC USA;
3.ScitoVation, Res Triangle Pk, NC USA;
4.Kelly Govt Solut, Res Triangle Pk, NC USA;
5.US EPA, Natl Exposure Res Lab, Off Res & Dev, Res Triangle Pk, NC 27711 USA
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GB/T 7714
Casey, Warren M.,Chang, Xiaoqing,Allen, David G.,et al. Evaluation and Optimization of Pharmacokinetic Models for in Vitro to in Vivo Extrapolation of Estrogenic Activity for Environmental Chemicals[J]. ENVIRONMENTAL HEALTH PERSPECTIVES,2018,126(9).
APA Casey, Warren M..,Chang, Xiaoqing.,Allen, David G..,Ceger, Patricia C..,Choksi, Neepa Y..,...&Kleinstreuer, Nicole C..(2018).Evaluation and Optimization of Pharmacokinetic Models for in Vitro to in Vivo Extrapolation of Estrogenic Activity for Environmental Chemicals.ENVIRONMENTAL HEALTH PERSPECTIVES,126(9).
MLA Casey, Warren M.,et al."Evaluation and Optimization of Pharmacokinetic Models for in Vitro to in Vivo Extrapolation of Estrogenic Activity for Environmental Chemicals".ENVIRONMENTAL HEALTH PERSPECTIVES 126.9(2018).
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