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新生儿中基因变异对对氧磷酶1(PON1)活性的影响增强。

Increased influence of genetic variation on PON1 activity in neonates.

作者信息

Chen Jia, Kumar Madhu, Chan Wendy, Berkowitz Gertrud, Wetmur James G

机构信息

The Derald H. Ruttenberg Cancer Center, and Department of Community and Preventive Medicine, Mount Sinai School of Medicine, New York, New York 10029, USA.

出版信息

Environ Health Perspect. 2003 Aug;111(11):1403-9. doi: 10.1289/ehp.6105.

Abstract

PON1 (paraoxonase-1) detoxifies organophosphates by cleavage of active oxons before they have a chance to inhibit cholinesterases. The corresponding gene PON1 has common polymorphisms in both the promoter (-909, -162, -108) and the coding region (L55M, Q192R). The five PON1 genotypes were determined for maternal blood (n= 402) and cord blood (n= 229) as part of a study of the effects of organophosphate pesticide exposure on infant growth and neurodevelopment. PON1 enzymatic activities were determined for a majority of subjects. The population contained Caucasians, Caribbean Hispanics, and African Americans. PON1 activity was strongly dependent upon the promoter alleles in both maternal and cord blood. For example, PON1 activities for position -108CC, CT, and TT mothers were 146, 128, and 109 arylesterase U/mL (analysis of variance, p< 0.0001), whereas the same PON1 activities for the respective cord bloods were 49.0, 32.4, and 23.2 U/mL (p < 0.0001). Compared with adults, neonates had lower PON1 activity, implying reduced capacity to detoxify organophosphates. In addition there was a larger difference in activity between genotype groups in neonates than in adults. Because the five polymorphisms in PON1 occur in a short stretch of DNA, they were tested for linkage disequilibrium (LD). Significant LD was found among all three promoter polymorphisms as well as between promoter polymorphisms and L55M, with the strongest LD for Caucasians and the weakest for African Americans. The Caribbean Hispanics fall between these two groups. Surprisingly, significant LD also was observed between the promoter polymorphisms and C311S in PON2. LD between the promoter polymorphisms and Q192R was not significant.

摘要

对氧磷酶1(PON1)通过在活性氧肟酸有机会抑制胆碱酯酶之前将其裂解来解毒有机磷酸酯。相应的基因PON1在启动子(-909、-162、-108)和编码区(L55M、Q192R)都有常见的多态性。作为有机磷酸酯农药暴露对婴儿生长和神经发育影响研究的一部分,对402份母体血液和229份脐带血样本测定了五种PON1基因型。对大多数受试者测定了PON1酶活性。研究人群包括高加索人、加勒比西班牙裔和非裔美国人。PON1活性在母体血液和脐带血中都强烈依赖于启动子等位基因。例如,-108位点CC、CT和TT基因型母亲的PON1活性分别为146、128和109芳基酯酶U/mL(方差分析,p<0.0001),而相应脐带血中的PON1活性分别为49.0、32.4和23.2 U/mL(p<0.0001)。与成年人相比,新生儿的PON1活性较低,这意味着其解毒有机磷酸酯的能力较低。此外,新生儿基因型组之间的活性差异比成年人更大。由于PON1中的五个多态性出现在一段较短的DNA片段中,因此对它们进行了连锁不平衡(LD)测试。在所有三个启动子多态性之间以及启动子多态性与L55M之间都发现了显著的LD,其中高加索人的LD最强,非裔美国人的LD最弱。加勒比西班牙裔介于这两组之间。令人惊讶的是,在启动子多态性与PON2中的C311S之间也观察到了显著的LD。启动子多态性与Q192R之间的LD不显著。

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