瘦素受体基因座的拷贝数变异与代谢特征和 2 型糖尿病风险相关。
Copy number variation at leptin receptor gene locus associated with metabolic traits and the risk of type 2 diabetes mellitus.
机构信息
Division of Biobank for Health Sciences, Korea National Institute of Health, Korea Centers for Disease Control and Prevention, 194 Tongil Ro, Seoul, 122-701, Korea.
出版信息
BMC Genomics. 2010 Jul 12;11:426. doi: 10.1186/1471-2164-11-426.
BACKGROUND
Recent efforts have been made to link complex human traits and disease susceptibility to DNA copy numbers. The leptin receptor (LEPR) has been implicated in obesity and diabetes. Mutations and genetic variations of LEPR gene have been discovered in rodents and humans. However, the association of DNA copy number variations at the LEPR gene locus with human complex diseases has not been reported. In an attempt to study DNA copy number variations associated with metabolic traits and type 2 diabetes mellitus (T2DM), we targeted the LEPR gene locus in DNA copy number analyses.
RESULTS
We identified DNA copy number variations at the LEPR gene locus among a Korean population using genome-wide SNP chip data, and then quantified copy numbers of the E2 DNA sequence in the first two exons overlapped between LEPR and LEPROT genes by the quantitative multiplex PCR of short fluorescent fragment (QMPSF) method. Among the non-diabetic subjects (n = 1,067), lower E2 DNA copy numbers were associated with higher fasting glucose levels in men (p = 1.24 x 10(-7)) and women (p = 9.45 x 10(-5)), as well as higher total cholesterol levels in men (p = 9.96 x 10(-7)). In addition, the significant association between lower E2 DNA copy numbers and lower level of postprandial 2 hr insulin was evident only in non-diabetic women, whereas some obesity-related phenotypes and total cholesterol level exhibited significant associations only in non-diabetic men. Logistic regression analysis indicated that lower E2 DNA copy numbers were associated with T2DM (odds ratio, 1.92; 95% CI, 1.26-2.96; p < 0.003) in our nested case-control study. Interestingly, the E2 DNA copy number exhibited a negative correlation with LEPR gene expression, but a positive correlation with LEPROT gene expression.
CONCLUSIONS
This work suggests that a structural variation at the LEPR gene locus is functionally associated with complex metabolic traits and the risk of T2DM.
背景
最近的研究努力将复杂的人类特征和疾病易感性与 DNA 拷贝数联系起来。瘦素受体 (LEPR) 已被牵连到肥胖和糖尿病中。在啮齿动物和人类中已发现 LEPR 基因的突变和遗传变异。然而,LEPR 基因座处的 DNA 拷贝数变异与人类复杂疾病的关联尚未报道。为了研究与代谢特征和 2 型糖尿病 (T2DM) 相关的 DNA 拷贝数变异,我们在 DNA 拷贝数分析中以 LEPR 基因座为目标。
结果
我们使用全基因组 SNP 芯片数据在韩国人群中鉴定了 LEPR 基因座处的 DNA 拷贝数变异,然后通过定量多重 PCR 短荧光片段 (QMPSF) 方法定量了 LEPR 和 LEPROT 基因之间前两个外显子重叠的 E2 DNA 序列的拷贝数。在非糖尿病受试者(n = 1,067)中,男性(p = 1.24 x 10(-7)) 和女性(p = 9.45 x 10(-5))空腹血糖水平较高的 E2 DNA 拷贝数较低,男性总胆固醇水平较高(p = 9.96 x 10(-7))。此外,仅在非糖尿病女性中,E2 DNA 拷贝数较低与餐后 2 小时胰岛素水平较低之间存在显著关联,而一些肥胖相关表型和总胆固醇水平仅在非糖尿病男性中存在显著关联。逻辑回归分析表明,在我们的嵌套病例对照研究中,E2 DNA 拷贝数较低与 T2DM 相关(优势比,1.92;95%CI,1.26-2.96;p < 0.003)。有趣的是,E2 DNA 拷贝数与 LEPR 基因表达呈负相关,与 LEPROT 基因表达呈正相关。
结论
这项工作表明,LEPR 基因座处的结构变异与复杂代谢特征和 T2DM 的风险具有功能相关性。
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