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ERAP2 基因与澳大利亚和挪威人群的子痫前期有关。

The ERAP2 gene is associated with preeclampsia in Australian and Norwegian populations.

机构信息

Department of Genetics, Southwest Foundation for Biomedical Research, San Antonio, TX 78227, USA.

出版信息

Hum Genet. 2009 Nov;126(5):655-66. doi: 10.1007/s00439-009-0714-x. Epub 2009 Jul 4.

Abstract

Preeclampsia is a heritable pregnancy disorder that presents new onset hypertension and proteinuria. We have previously reported genetic linkage to preeclampsia on chromosomes 2q, 5q and 13q in an Australian/New Zealand (Aust/NZ) familial cohort. This current study centered on identifying the susceptibility gene(s) at the 5q locus. We first prioritized candidate genes using a bioinformatic tool designed for this purpose. We then selected a panel of known SNPs within ten prioritized genes and genotyped them in an extended set of the Aust/NZ families and in a very large, independent Norwegian case/control cohort (1,139 cases, 2,269 controls). In the Aust/NZ cohort we identified evidence of a genetic association for the endoplasmic reticulum aminopeptidase 1 (ERAP1) gene (rs3734016, P (uncorr) = 0.009) and for the endoplasmic reticulum aminopeptidase 2 (ERAP2) gene (rs2549782, P (uncorr) = 0.004). In the Norwegian cohort we identified evidence of a genetic association for ERAP1 (rs34750, P (uncorr) = 0.011) and for ERAP2 (rs17408150, P (uncorr) = 0.009). The ERAP2 SNPs in both cohorts remained statistically significant (rs2549782, P (corr) = 0.018; rs17408150, P (corr) = 0.039) after corrections at an experiment-wide level. The ERAP1 and ERAP2 genes encode enzymes that are reported to play a role in blood pressure regulation and essential hypertension in addition to innate immune and inflammatory responses. Perturbations within vascular, immunological and inflammatory pathways constitute important physiological mechanisms in preeclampsia pathogenesis. We herein report a novel preeclampsia risk locus, ERAP2, in a region of known genetic linkage to this pregnancy-specific disorder.

摘要

子痫前期是一种遗传性妊娠疾病,表现为新发生的高血压和蛋白尿。我们之前曾在澳大利亚/新西兰(Aust/NZ)家族队列中报告过染色体 2q、5q 和 13q 上与子痫前期相关的遗传连锁。本研究集中于鉴定 5q 基因座上的易感基因。我们首先使用为此目的设计的生物信息学工具对候选基因进行优先级排序。然后,我们在一个扩展的 Aust/NZ 家族和一个非常大的、独立的挪威病例/对照队列(1139 例病例,2269 例对照)中选择了十个优先基因内的已知 SNPs 进行基因分型。在 Aust/NZ 队列中,我们发现内质网氨肽酶 1(ERAP1)基因(rs3734016,P(uncorr)=0.009)和内质网氨肽酶 2(ERAP2)基因(rs2549782,P(uncorr)=0.004)存在遗传关联的证据。在挪威队列中,我们发现 ERAP1(rs34750,P(uncorr)=0.011)和 ERAP2(rs17408150,P(uncorr)=0.009)存在遗传关联的证据。两个队列中的 ERAP2 SNP 仍然具有统计学意义(rs2549782,P(corr)=0.018;rs17408150,P(corr)=0.039),经过全实验水平的校正。ERAP1 和 ERAP2 基因编码的酶被报道在血压调节和原发性高血压中发挥作用,此外还在先天免疫和炎症反应中发挥作用。血管、免疫和炎症途径中的紊乱是子痫前期发病机制中的重要生理机制。本研究在该妊娠特异性疾病的已知遗传连锁区域中报告了一个新的子痫前期风险基因座 ERAP2。

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