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Detection of novel genetic markers of susceptibility to preeclampsia based on an analysis of the regulatory genes in the placental tissue

机译:基于胎盘组织中调控基因的分析,检测子痫前期易感性的新遗传标记

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摘要

Regulatory single nucleotide polymorphisms (rSNPs) are the least-studied group of SNP; however, they play an essential role in the development of human pathology by altering the level of candidate genes expression. In this work, we analyzed 29 rSNPs in 17 new candidate genes associated with preeclampsia (PE) according to the analysis of the transcriptome in placental tissue. Three ethnic groups have been studied (Yakut, Russian, and Buryat). We have detected significant associations of PE with eight rSNPs in six differentially expressed genes, i.e., rs10423795 in the LHB gene; rs3771787 in the HK2 gene; rs72959687 in the INHA gene; rs12678229, rs2227262, and rs3802252 in the NDRG1 gene; rs34845949 in the SASH1 gene; and rs66707428 in the PPP1R12C gene. We used a new approach to detecting genetic markers of multifactorial diseases in the case of PE based on a combination of genomic, transcriptomic, and bioinformatic approaches. This approach proved its efficiency and may be applied to detecting new potential genetic markers in genes involved in disease pathogenesis, which reduces missing heritability in multifactorial diseases.
机译:调节性单核苷酸多态性(rSNPs)是研究最少的SNP组。然而,它们通过改变候选基因的表达水平在人类病理学发展中起着至关重要的作用。在这项工作中,我们根据胎盘组织中转录组的分析,分析了与子痫前期(PE)相关的17个新候选基因中的29个rSNP。研究了三个民族(雅库特,俄罗斯和布里亚特)。我们已经在六个差异表达的基因(即LHB基因中的rs10423795)中检测到PE与八个rSNP的显着关联; HK2基因中的rs3771787; INHA基因中的rs72959687; NDRG1基因中的rs12678229,rs2227262和rs3802252; SASH1基因中的rs34845949;和rs66707428位于PPP1R12C基因中。在基因组,转录组学和生物信息学方法相结合的基础上,我们采用了一种新方法来检测PE病例中多因素疾病的遗传标记。该方法证明了其有效性,可用于检测与疾病发病机理有关的基因中新的潜在遗传标记,从而降低多因素疾病中遗漏的遗传力。

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