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白色丹麦人群中GNB3 825C>T基因多态性与代谢综合征各组分相关性的研究。

Studies of the association of the GNB3 825C>T polymorphism with components of the metabolic syndrome in white Danes.

作者信息

Andersen G, Overgaard J, Albrechtsen A, Glümer C, Borch-Johnsen K, Jørgensen T, Hansen T, Pedersen O

机构信息

Steno Diabetes Center, Niels Steensens Vej 2, NSH2.16, 2820 Gentofte, Denmark.

出版信息

Diabetologia. 2006 Jan;49(1):75-82. doi: 10.1007/s00125-005-0049-7. Epub 2005 Nov 12.

Abstract

AIMS/HYPOTHESIS: The 825C>T polymorphism in the gene encoding the G protein beta3 subunit (GNB3) causes enhanced G protein activation and increased in vitro cell proliferation. This polymorphism is also repeatedly associated with an increased risk of hypertension and has been studied in relation to obesity with divergent results. Only a few association studies have investigated whether this polymorphism is related to type 2 diabetes or the metabolic syndrome. We estimated the impact of the GNB3 825C>T polymorphism in relatively large-scale association studies of common phenotypes of the metabolic syndrome.

MATERIALS AND METHODS

The GNB3 825C>T polymorphism was genotyped in 7,518 white Danish subjects using mass spectrometry analysis of PCR products. Case-control studies were undertaken for obesity, hypertension, type 2 diabetes and the metabolic syndrome, and a meta-analysis including data from the present study and previous studies of hypertension was performed. Quantitative trait studies of metabolic variables were carried out in 4,387 glucose-tolerant subjects.

RESULTS

We observed minor differences in 825C>T genotype distributions for type 2 diabetes (CC/CT/TT 49/41/10% (control) vs 46/46/9% (cases), respectively, p=0.007); however, after correction for multiple testing, these were not statistically significant. No association was found with hypertension, obesity or the metabolic syndrome. Curiously, the T allele was associated with nominally lower systolic and diastolic blood pressure levels-a finding in contrast with most previous studies-but not with other metabolic variables. Meta-analysis demonstrated a high degree of heterogeneity between study populations of different ethnic origin. Although there was a tendency towards an increased risk of hypertension among 825T allele carriers, this was not statistically significant.

CONCLUSIONS/INTERPRETATION: The present study suggests no major involvement of the GNB3 825C>T polymorphism in components of the metabolic syndrome.

摘要

目的/假设:编码G蛋白β3亚基(GNB3)的基因中的825C>T多态性导致G蛋白激活增强和体外细胞增殖增加。这种多态性还反复与高血压风险增加相关,并且已经针对肥胖进行了研究,但结果不一。只有少数关联研究调查了这种多态性是否与2型糖尿病或代谢综合征有关。我们在相对大规模的代谢综合征常见表型关联研究中评估了GNB3 825C>T多态性的影响。

材料与方法

采用PCR产物质谱分析法对7518名丹麦白人受试者的GNB3 825C>T多态性进行基因分型。针对肥胖、高血压、2型糖尿病和代谢综合征进行病例对照研究,并对本研究数据和既往高血压研究数据进行荟萃分析。在4387名糖耐量正常的受试者中进行代谢变量的定量性状研究。

结果

我们观察到2型糖尿病患者825C>T基因型分布存在微小差异(CC/CT/TT分别为49/41/10%(对照组)和46/46/9%(病例组),p=0.007);然而,在进行多重检验校正后,这些差异无统计学意义。未发现与高血压、肥胖或代谢综合征有关联。奇怪的是,T等位基因与名义上较低的收缩压和舒张压水平相关——这一发现与大多数既往研究相反——但与其他代谢变量无关。荟萃分析表明不同种族来源的研究人群之间存在高度异质性。尽管825T等位基因携带者患高血压的风险有增加趋势,但无统计学意义。

结论/解读:本研究表明GNB3 825C>T多态性在代谢综合征各组分中无主要作用。

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