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Influence of Endothelial Nitric Oxide Synthase Gene Intron-4 27bp Repeat Polymorphism on Its Expression in Autoimmune Diseases

机译:内皮型一氧化氮合酶基因Intron-4 27bp重复多态性对其自身免疫性疾病表达的影响

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摘要

The purpose of this study was to analyse the effect of the T-786C polymorphism and intron 4 27 bp variable number tandem repeat(VNTR) eNOS markers for their potential association with Systemic Lupus Erythematosus(SLE), Hashimotos thyroiditis(HT) and Rheumatoid arthritis(RA) as well as to explore their effect on eNOS mRNA expression and nitrate production(NOx). Kuwaitis (n = 383) matched by age, gender and ethnicity were genotyped by fluorescent-labelled-restriction fragment length polymorphism (RFLP) and fragment analysis. Expression of eNOS mRNA was analysed using RT-PCR and sera from subjects were screened for NOx using ELISA. Analysis of the allelic frequency revealed a significant association of the 4b allele with susceptibility to SLE (p = 0.0092, OR = 1.76). The 4bb genotype was found to be associated with SLE (p = 0.0076, OR = 1.97) and HT (p = 0.05, OR = 1.81). Allelic and genotypic distribution did not differ between RA patients and healthy control subjects. The 4bb genotype resulted in reduced expression of eNOS mRNA in SLE, RA and HT, but only the reduction in HT was significant (p = 0.05). The 4ab genotype revealed a significant association with increased eNOS expression in HT (p = 0.03) and RA (p = 0.014) patients, and elevated NOx levels were detected in the autoimmune disease cohorts (p < 0.05) when compared to healthy control subjects. The T-786C SNP failed to show a significant association (p > 0.05) with SLE, HT, and RA patients. This study is the first to reveal a significant association between the 4bb genotype of the 27 bp VNTR and susceptibility to HT. The expression of eNOS is related to the number of 27 bp repeats, with heterozygous 4bb repeats showing a decrease in eNOS expression. eNOS – endothelial nitric oxide synthase.
机译:这项研究的目的是分析T-786C多态性和内含子4 27 bp可变数目串联重复重复(VNTR)eNOS标记与系统性红斑狼疮(SLE),桥本甲状腺炎(HT)和类风湿关节炎的潜在关联的作用(RA)并探讨其对eNOS mRNA表达和硝酸盐生成(NOx)的影响。根据年龄,性别和种族匹配的科威特人(n = 383)通过荧光标记限制性片段长度多态性(RFLP)和片段分析进行基因分型。使用RT-PCR分析eNOS mRNA的表达,并使用ELISA筛选受试者血清中的NOx。对等位基因频率的分析表明,4b等位基因与对SLE的敏感性显着相关(p = 0.0092,OR = 1.76)。发现4bb基因型与SLE(p = 0.0076,OR = 1.97)和HT(p = 0.05,OR = 1.81)相关。 RA患者与健康对照组之间的等位基因和基因型分布没有差异。 4bb基因型导致eNOS mRNA在SLE,RA和HT中的表达降低,但只有HT的降低显着(p = 0.05)。 4ab基因型显示与HT(p = 0.03)和RA(p = 0.014)患者的eNOS表达增加显着相关,并且与健康对照组相比,自身免疫性疾病队列中检测到的NOx水平升高(p <0.05)。 T-786C SNP与SLE,HT和RA患者没有显着相关性(p> 0.05)。这项研究是第一个揭示27 bp VNTR的4bb基因型与HT敏感性之间显着关联的研究。 eNOS的表达与27 bp重复的数目有关,杂合的4bb重复显示eNOS表达的减少。 eNOS –内皮型一氧化氮合酶。

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