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Glycated Serum Protein Genetics and Pleiotropy with Cardiometabolic Risk Factors

机译:糖化血清蛋白遗传学和多向性与心脏代谢危险因素

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摘要

Measurements of fasting glucose (FG) or glycated hemoglobin A1c (HbA1c) are two clinically approved approaches commonly used to determine glycemia, both of which are influenced by genetic factors. Obtaining accurate measurements of FG or HbA1c is not without its challenges, though. Measuring glycated serum protein (GSP) offers an alternative approach for assessing glycemia. The aim of this study was to estimate the heritability of GSP and GSP expressed as a percentage of total serum albumin (%GA) using a variance component approach and localize genomic regions (QTLs) that harbor genes likely to influence GSP and %GA trait variation in a large extended multigenerational pedigree from Jiri, Nepal (n = 1,800). We also performed quantitative bivariate analyses to assess the relationship between GSP or %GA and several cardiometabolic traits. Additive genetic effects significantly influence variation in GSP and %GA levels (p values: 1.15 × 10−5 and 3.39 × 10−5, respectively). We localized a significant (LOD score = 3.18) and novel GSP QTL on chromosome 11q, which has been previously linked to type 2 diabetes. Two common (MAF > 0.4) SNPs within the chromosome 11 QTL were associated with GSP (adjusted pvalue < 5.87 × 10−5): an intronic variant (rs10790184) in the DSCAML1 gene and a 3′UTR variant (rs8258) in the CEP164 gene. Significant positive correlations were observed between GSP or %GA and blood pressure, and lipid traits (p values: 0.0062 to 1.78 × 10−9). A significant negative correlation was observed between %GA and HDL cholesterol (p = 1.12 × 10−5). GSP is influenced by genetic factors and can be used to assess glycemia and diabetes risk. Thus, GSP measurements can facilitate glycemic studies when accurate FG and/or HbA1c measurements are difficult to obtain. GSP can also be measured from frozen blood (serum) samples, which allows the prospect of retrospective glycemic studies using archived samples.
机译:空腹血糖(FG)或糖化血红蛋白A1c(HbA1c)的测量是两种常用的确定血糖的临床认可方法,这两种方法均受遗传因素影响。但是,获得FG或HbA1c的准确测量并非没有挑战。测量糖化血清蛋白(GSP)提供了另一种评估血糖的方法。这项研究的目的是使用方差成分方法估算GSP和GSP的遗传力,以总血清白蛋白(%GA)的百分比表示,并定位可能包含可能影响GSP和%GA性状变异的基因的基因组区域(QTL)来自尼泊尔吉里(n = 1,800)的大型多代谱系。我们还进行了定量双变量分析,以评估GSP或%GA与几种心脏代谢特征之间的关系。加性遗传效应显着影响GSP和%GA水平的变化(p值分别为1.15×10 −5 和3.39×10 −5 )。我们在染色体11q上定位了一个显着(LOD分数= 3.18)和新颖的GSP QTL,该染色体先前与2型糖尿病有关。 11个QTL染色体中的两个常见(MAF> 0.4)SNP与GSP相关(调整后的pvalue <5.87×10 -5 ):DSCAML1基因的一个内含子变体(rs10790184)和一个3'UTR CEP164基因中的变体(rs8258)。 GSP或%GA与血压和血脂性状之间存在显着正相关(p值:0.0062至1.78×10 −9 )。 %GA与HDL胆固醇之间存在显着的负相关(p = 1.12×10 -5 )。 GSP受遗传因素影响,可用于评估血糖和糖尿病风险。因此,当难以获得准确的FG和/或HbA1c测量值时,GSP测量值可以帮助进行血糖研究。 GSP也可以从冷冻血液(血清)样本中进行测量,从而可以使用存档样本进行回顾性血糖研究。

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