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贝叶斯元分析人类血清对氧磷酶 1 活性表型差异在化学风险评估中的作用。

Bayesian meta-analysis of inter-phenotypic differences in human serum paraoxonase-1 activity for chemical risk assessment.

机构信息

Risk Assessment Department, French Agency for Food, Environmental and Occupational Health & Safety (ANSES), 14 rue Pierre et Marie Curie, Maisons-Alfort F-94700, France.

Institute for Risk Assessment Sciences, Utrecht University, 3508 TD Utrecht, the Netherlands.

出版信息

Environ Int. 2020 May;138:105609. doi: 10.1016/j.envint.2020.105609. Epub 2020 Feb 27.

Abstract

Human variability in paraoxonase-1 (PON1) activities is driven by genetic polymorphisms that affect the internal dose of active oxons of organophosphorus (OP) insecticides. Here, an extensive literature search has been performed to collect human genotypic frequencies (i.e. L55M, Q192R, and C-108T) in subgroups from a range of geographical ancestry and PON1 activities in three probe substrates (paraoxon, diazoxon and phenyl acetate). Bayesian meta-analyses were performed to estimate variability distributions for PON1 activities and PON1-related uncertainty factors (UFs), while integrating quantifiable sources of inter-study, inter-phenotypic and inter-individual differences. Inter-phenotypic differences were quantified using the population with high PON1 activity as the reference group. Results from the meta-analyses provided PON1 variability distributions and these can be implemented in generic physiologically based kinetic models to develop quantitative in vitro in vivo extrapolation models. PON1-related UFs in the Caucasian population were above the default toxicokinetic UF of 3.16 for two specific genotypes namely -108CC using diazoxon as probe substrate and, -108CT, -108TT, 55MM and 192QQ using paraoxon as probe substrate. However, integration of PON1 genotypic frequencies and activity distributions showed that all UFs were within the default toxicokinetic UF. Quantitative inter-individual differences in PON1 activity are important for chemical risk assessment particularly with regards to the potential sensitivity to organophosphates' toxicity.

摘要

人对paraoxonase-1(PON1)活性的个体差异是由遗传多态性引起的,这些多态性影响有机磷(OP)杀虫剂活性氧的内剂量。在此,通过广泛的文献检索,收集了来自不同地理背景的亚组人群的PON1 基因型频率(即 L55M、Q192R 和 C-108T)和三种探针底物(对氧磷、二嗪农和苯乙酸酯)中的 PON1 活性。进行贝叶斯荟萃分析以估计 PON1 活性和 PON1 相关不确定性因素(UF)的变异性分布,同时整合可量化的研究间、表型间和个体间差异来源。使用高 PON1 活性人群作为参考组来量化表型间差异。荟萃分析的结果提供了 PON1 变异性分布,这些分布可用于通用的基于生理学的动力学模型中,以开发定量的体外体内外推模型。在白种人群中,PON1 相关 UF 高于默认的毒代动力学 UF3.16,对于两种特定基因型 -108CC(使用二嗪农作为探针底物)和 -108CT、-108TT、55MM 和 192QQ(使用对氧磷作为探针底物)。然而,PON1 基因型频率和活性分布的整合表明,所有 UF 均在默认毒代动力学 UF 范围内。PON1 活性的定量个体间差异对于化学风险评估很重要,特别是对于有机磷毒性的潜在敏感性。

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