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Diplotype analysis of the human cardiac sodium channel regulatory region in Japanese cases of sudden death by unknown causes.

机译:在日本人死于不明原因的案例中,人类心脏钠通道调节区的双型分析。

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Inherited mutations in the human cardiac sodium channel (SCN5A) gene cause arrhythmogenic diseases such as tachyarrhythmia and bradyarrhythmia. Moreover, mutation subsets in the coding region impair SCN5A function, potentially leading to sudden cardiac death (SCD). In the present study, we performed diplotype analysis of the regulatory region of the SCN5A gene in Japanese people who died suddenly because of an unknown cause (sudden death group; n=70) and controls (n=112). There were no significant differences at six polymorphic loci between the groups. However, 38 diplotypes of 6-nucleotide polymorphism variants were identified. One of these diplotypes-Dip.D (CTG-TC/CCG-TC)-occurred significantly more frequently in the sudden death group than in the controls (p<0.01, OR=5.18, 95% CI: 1.38-19.45). Dip.D has two variants (T-1062C and T-847G), and while it is unclear whether these directly affect mRNA expression, a common polymorphism in this region modulates SCN5A expression in vitro. Our results thus suggest that the transcription of the SCN5A Dip.D variant may be associated with arrhythmogenic diseases that can induce sudden death.
机译:人的心脏钠通道(SCN5A)基因中的遗传突变会导致心律失常性疾病,例如心律失常和心律失常。此外,编码区中的突变子集会损害SCN5A功能,从而可能导致心脏性猝死(SCD)。在本研究中,我们对因未知原因(猝死组; n = 70)和对照组(n = 112)而突然死亡的日本人进行了SCN5A基因调控区的双型分析。两组之间的六个多态性位点没有显着差异。然而,鉴定出38种6-核苷酸多态性变体的双倍型。这些双倍型之一-Dip.D(CTG-TC / CCG-TC)-在猝死组中的发生率明显高于对照组(p <0.01,OR = 5.18,95%CI:1.38-19.45)。 Dip.D具有两个变体(T-1062C和T-847G),虽然尚不清楚它们是否直接影响mRNA表达,但该区域的常见多态性在体外调节SCN5A表达。因此,我们的结果表明,SCN5A Dip.D变体的转录可能与可导致猝死的心律失常疾病相关。

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