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对氧磷酶 1(PON1)的遗传多态性:PON1 活性的人群分布。

Genetic polymorphism in paraoxonase 1 (PON1): Population distribution of PON1 activity.

机构信息

Connecticut Department of Public Health, Hartford, 06134, USA.

出版信息

J Toxicol Environ Health B Crit Rev. 2009;12(5-6):473-507. doi: 10.1080/10937400903158409.

Abstract

Paraoxonase-1 (PON1) is a serum esterase that hydrolyzes the activated oxon form of several organophosphates. The central role of PON1 in detoxification of organophosphate (OP) pesticides was demonstrated in knockout mouse studies, suggesting that human variability in PON1 needs to be considered in health risk assessments involving exposure to these pesticides. The current analysis focused on two genetic loci in which polymorphisms demonstrated to affect PON1 activity. Detailed kinetic studies and population studies found that the *192Q (wild type) allele is more active toward some substrates (such as sarin, soman, and diazoxon) and less active toward others (such as paraoxon or chlorpyrifos) relative to the variant *192R allele. Another allele that affects activity is *55M; PON1 enzyme quantity, rather than specific activity or substrate preference, is altered. The *192R variant occurs commonly with a frequency of 25-64% across the populations analyzed. The *55M allele is less common, occurring in 5-40% of individuals depending upon the ethnic group studied. These activity and allele frequency data were incorporated into Monte Carlo simulations in which the frequency of both variant alleles was simultaneously modeled in Caucasian, African American, and Japanese populations. The resulting Monte Carlo activity distributions were bimodal for the substrate paraoxon with approximately fourfold differences between low- and high-activity modal medians. Differences in activity between total population median and 1st percentile were five- to sixfold. When sarin metabolic variability was simulated, the population distributions were unimodal. However, there was an even greater degree of interindividual variability (median to 1st percentile difference >20-fold). These results show that the combined effects of two PON1 allelic variants yielded a population distribution that is associated with a considerable degree of interindividual variability in enzyme activity. This indicates that assessments involving PON1 substrates need to evaluate polymorphism-related variability in enzyme activity to display the distribution of internal doses and adverse responses. This may best be achieved via physiologically based pharmacokinetic (PBPK) models that input PON1 activity distributions, such as those generated in this analysis, to simulate the range of oxon internal doses possible across the population.

摘要

对氧磷酶 1(PON1)是一种血清酯酶,可水解几种有机磷酸酯的活化氧肟形式。在敲除小鼠研究中,PON1 在有机磷(OP)农药解毒中的核心作用得到了证实,这表明在涉及接触这些农药的健康风险评估中,需要考虑人类 PON1 的变异性。目前的分析集中在两个遗传位点上,其中已证明多态性会影响 PON1 活性。详细的动力学研究和人群研究发现,相对于变体 *192R 等位基因,192Q(野生型)等位基因对某些底物(如沙林、梭曼和敌敌畏)更活跃,而对其他底物(如对氧磷或毒死蜱)的活性较低。另一个影响活性的等位基因是55M;改变的是 PON1 酶的数量,而不是特定的活性或底物偏好。*192R 变体在分析的人群中普遍存在,频率为 25-64%。*55M 等位基因较少见,在 5-40%的个体中存在,具体取决于所研究的种族群体。这些活性和等位基因频率数据被纳入蒙特卡罗模拟中,其中在白种人、非裔美国人和日本人中同时对两个变体等位基因的频率进行建模。模拟物对氧磷的蒙特卡罗活性分布呈双峰分布,低活性模态中位数和高活性模态中位数之间的差异约为四倍。总人群中位数和第 1 百分位数之间的活性差异为五到六倍。模拟沙林代谢变异性时,人群分布呈单峰分布。然而,个体间的变异性更大(中位数与第 1 百分位数的差异>20 倍)。这些结果表明,两个 PON1 等位基因变异的综合效应产生了一种与酶活性个体间差异相当大的人群分布。这表明,涉及 PON1 底物的评估需要评估与酶活性相关的多态性变异,以显示内部剂量和不良反应的分布。这可能通过生理相关的药代动力学(PBPK)模型来实现,这些模型输入 PON1 活性分布,例如本分析中生成的分布,以模拟人群中可能存在的氧化内部剂量范围。

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