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首页> 外文期刊>Metabolism: Clinical and Experimental >Genome-wide association study identifies common loci influencing circulating glycated hemoglobin (HbA1c) levels in non-diabetic subjects: The Long Life Family Study (LLFS)
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Genome-wide association study identifies common loci influencing circulating glycated hemoglobin (HbA1c) levels in non-diabetic subjects: The Long Life Family Study (LLFS)

机译:全基因组关联研究确定了影响非糖尿病患者循环糖化血红蛋白(HbA1c)水平的常见基因座:长寿命家庭研究(LLFS)

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Objective Glycated hemoglobin (HbA1c) is a stable index of chronic glycemic status and hyperglycemia associated with progressive development of insulin resistance and frank diabetes. It is also associated with premature aging and increased mortality. To uncover novel loci for HbA 1c that are associated with healthy aging, we conducted a genome-wide association study (GWAS) using non-diabetic participants in the Long Life Family Study (LLFS), a study with familial clustering of exceptional longevity in the US and Denmark. Methods A total of 4088 non-diabetic subjects from the LLFS were used for GWAS discoveries, and a total of 8231 non-diabetic subjects from the Atherosclerosis Risk in Communities Study (ARIC, in the MAGIC Consortium) and the Health, Aging, and Body Composition Study (HABC) were used for GWAS replications. HbA1c was adjusted for age, sex, centers, 20 principal components, without and with BMI. A linear mixed effects model was used for association testing. Results Two known loci at GCK rs730497 (or rs2908282) and HK1 rs17476364 were confirmed (p 5e-8). Of 25 suggestive (5e-8 p 1e-5) loci, one known (G6PC2 rs560887, replication p = 5e-5) and one novel (OR10R3P/SPTA1 - rs12041363, replication p = 1e-17) loci were replicated (p 0.0019). Similar findings resulted when HbA1c was further adjusted for BMI. Further validations are crucial for the remaining suggestive loci including the emerged variant near OR10R3P/SPTA1. Conclusions The analysis reconfirmed two known GWAS loci (GCK, HK1) and identified 25 suggestive loci including one reconfirmed variant in G6PC2 and one replicated variant near OR10R3P/SPTA1. Future focused survey of sequence elements containing mainly functional and regulatory variants may yield additional findings.
机译:目的糖化血红蛋白(HbA1c)是慢性血糖状态和高血糖症的稳定指标,与胰岛素抵抗和坦率糖尿病的进展有关。它还与过早衰老和死亡率增加有关。为了发现与健康衰老相关的HbA 1c的新基因座,我们使用长寿家庭研究(LLFS)中的非糖尿病参与者进行了全基因组关联研究(GWAS),该研究以长寿家族研究中的超长寿命家族聚类为研究对象。美国和丹麦。方法共有LLFS的4088名非糖尿病受试者用于GWAS发现,社区研究中的动脉粥样硬化风险(ARIC,MAGIC联盟)以及健康,老龄化和身体方面的8231名非糖尿病受试者成分研究(HABC)用于GWAS复制。调整HbA1c的年龄,性别,中心,20个主要成分(不包括BMI)。线性混合效应模型用于关联测试。结果确认在GCK rs730497(或rs2908282)和HK1 rs17476364的两个已知基因座(p <5e-8)。在25个提示性位点(5e-8 <1e-5)中,复制了一个已知(G6PC2 rs560887,复制p = 5e-5)和一个新的(OR10R3P / SPTA1- rs12041363,复制p = 1e-17)基因座( p <0.0019)。当HbA1c进一步调整BMI时,也会得到类似的发现。对于剩余的提示基因座,包括在OR10R3P / SPTA1附近出现的变异体,进一步的验证至关重要。结论分析再次确认了两个已知的GWAS基因座(GCK,HK1),并鉴定了25个提示基因座,包括一个在G6PC2中重新确认的变体和一个在OR10R3P / SPTA1附近的复制变体。未来重点研究主要包含功能性和调节性变异的序列元件可能会产生其他发现。

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