Laboratory of Human Molecular Genetics, Faculty of Medicine, University of Sfax, Tunisia.
Gene. 2013 Sep 15;527(1):75-81. doi: 10.1016/j.gene.2013.05.064. Epub 2013 Jun 7.
Leptin (LEP) gene is one of the most promising candidate genes for obesity. Previous studies have tested the association of polymorphisms in LEP gene with obesity and obesity-related metabolic biomarkers (anthropometric variables, glucose, insulin level, leptin level and lipid profile). However, the results of these studies were still controversial. To determine whether LEP gene is associated with obesity in Tunisian population, we performed a family-based association study between LEP polymorphisms and obesity and obesity-related metabolic biomarkers.
Seven single nucleotide polymorphisms (SNPs) in 5' region of LEP gene were genotyped in three consanguineous families including 33 individuals. The previously reported LEP SNPs (H1328084, H1328082, rs10487506, H1328081, H1328080, G-2548A and A19G) were evaluated by PCR-RFLP and direct sequencing methods. Single SNP association and haplotype association analyses were performed using the family-based association test (FBAT). To determine allele frequencies of these SNPs in general population, 52 unrelated individuals from the general Tunisian population were also analyzed.
Two SNPs showed significant associations with plasma leptin level (H1328084: A>G, Z=2.058, p=0.039; A19G: G>A, Z=2.058, p=0.039). When haplotypes were constructed with these two-markers, the risk AA haplotype (frequency 57.1%) was positively associated with plasma leptin level (Z=2.058, p=0.039). Moreover, SNPs H1328084 and A19G are predicted to modify transcription-factor binding sites.
Our study provided that two functional variants in 5' regulatory region of LEP gene are associated with plasma leptin level as a quantitative trait. It suggested that H1328084 and A19G have an important role in regulating plasma leptin level.
瘦素(LEP)基因是肥胖最有希望的候选基因之一。先前的研究已经测试了 LEP 基因多态性与肥胖和肥胖相关代谢生物标志物(人体测量变量、葡萄糖、胰岛素水平、瘦素水平和血脂谱)之间的关联。然而,这些研究的结果仍存在争议。为了确定 LEP 基因是否与突尼斯人群中的肥胖有关,我们在三个近亲家庭中进行了 LEP 多态性与肥胖和肥胖相关代谢生物标志物之间的基于家族的关联研究。
在包括 33 个人的三个近亲家庭中,对 LEP 基因 5' 区的 7 个单核苷酸多态性(SNP)进行了基因分型。先前报道的 LEP SNP(H1328084、H1328082、rs10487506、H1328081、H1328080、G-2548A 和 A19G)通过 PCR-RFLP 和直接测序方法进行评估。使用基于家族的关联检验(FBAT)进行单 SNP 关联和单倍型关联分析。为了确定这些 SNP 在一般人群中的等位基因频率,还对来自一般突尼斯人群的 52 个无关个体进行了分析。
两个 SNP 与血浆瘦素水平显著相关(H1328084:A>G,Z=2.058,p=0.039;A19G:G>A,Z=2.058,p=0.039)。当用这两个标记构建单倍型时,风险 AA 单倍型(频率 57.1%)与血浆瘦素水平呈正相关(Z=2.058,p=0.039)。此外,SNP H1328084 和 A19G 预测可修饰转录因子结合位点。
本研究表明,LEP 基因 5' 调控区的两个功能变体与作为定量性状的血浆瘦素水平相关。这表明 H1328084 和 A19G 在调节血浆瘦素水平方面具有重要作用。
