Physiology Research Centre, Department of Physiology, Isfahan University of Medical Sciences, Hezar jerib Avenue, Isfahan, Iran.
Mol Biol Rep. 2012 Mar;39(3):3355-60. doi: 10.1007/s11033-011-1105-7. Epub 2011 Jul 3.
Heme oxygenase-1 (HO-1) which is a rate-limiting enzyme in heme degradation processes shows a dinucleotide GT repeat in the promoter that alters the level of gene transcription. This study is aimed to assess the association of HO-1 gene promoter polymorphism and metabolic syndrome (MetS). A hundred and fifty two individuals, who were followed in Isfahan Cohort Study since 2001, were enrolled in this study. They consisted of 78 MetS patients and 74 controls without MetS. Blood samples were obtained from all participants and after extracting the genomic DNA, promoter sequence was determined by PCR-based genotyping. The serum levels of iron, ferritin and bilirubin were also measured in all subjects. The proportion of short and long allele frequency did not significantly differ in patients with metabolic syndrome compared to control group. In conclusion, the results showed that there is no significant difference between two groups in (GT)n repeat of HO-1 gene promoter. These findings suggest the insignificant role of genetic risk factors compared to environmental risk factors in the development of MetS.
血红素加氧酶-1(HO-1)是血红素降解过程中的限速酶,其启动子中存在一个二核苷酸 GT 重复序列,可改变基因转录水平。本研究旨在评估 HO-1 基因启动子多态性与代谢综合征(MetS)的相关性。152 名参与者于 2001 年开始参与伊斯法罕队列研究,本研究将他们纳入其中。这些参与者包括 78 名 MetS 患者和 74 名无 MetS 的对照者。所有参与者均采集血样,提取基因组 DNA 后,采用基于 PCR 的基因分型法确定启动子序列。所有受试者的血清铁、铁蛋白和胆红素水平也均进行了测量。与对照组相比,代谢综合征患者的短和长等位基因频率比例没有显著差异。总之,HO-1 基因启动子(GT)n 重复的结果显示两组之间没有显著差异。这些发现表明,与环境危险因素相比,遗传危险因素在 MetS 的发生发展中作用不大。
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