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β2-肾上腺素能受体基因多态性、年龄与心血管表型

Beta(2)-adrenergic receptor gene polymorphism, age, and cardiovascular phenotypes.

作者信息

Castellano Maurizio, Rossi Federica, Giacchè Mara, Perani Cristiano, Rivadossi Francesca, Muiesan Maria Lorenza, Salvetti Massimo, Beschi Marina, Rizzoni Damiano, Agabiti-Rosei Enrico

机构信息

Department of Medical and Surgical Sciences, University of Brescia, Italy.

出版信息

Hypertension. 2003 Feb;41(2):361-7. doi: 10.1161/01.hyp.0000052831.85600.79.

Abstract

Previous studies suggest that variants of the beta(2)-adrenergic receptor (ADRB2) may differently affect functional responses to adrenergic stimulation, thereby possibly modulating cardiovascular and metabolic phenotypes. We examined the hypothesis that G/R16 and Q/E27 polymorphism of ADRB2, or their haplotypes, may modulate blood pressure, cardiovascular structure, and function or metabolic cardiovascular risk factors in the general population. We examined a random sample of the general population (n=571; age, 35 to 64 years). Neither clinic nor 24-hour ambulatory blood pressure was significantly associated with ADRB2 genotypes in the overall population. Cardiac structure and function were also not influenced by ADRB2 polymorphism. After adjustment for potential confounders, association of the R16 allele with higher systolic blood pressure was observed in the subgroup of younger people (below age of 50 years). Haplotype analysis showed that higher blood pressure values were more specifically associated with the presence of R16-Q27. Younger people carrying the R16-Q27 haplotype also showed a trend toward lower heart rate, higher BMI, lower glycemia, and higher trygliceridemia, which is consistent with the hypothesis of a genetic predisposition to reduced cardiovascular and metabolic response to ADRB2 stimulation. This study does not provide evidence of a major role of ADRB2 gene variability in blood pressure modulation. However, association of ADRB2 polymorphism with cardiovascular and metabolic effects can be observed in younger subjects, before the development of age-related decline of ADRB2-mediated activity. Our study emphasizes the necessity of taking into account (patho)-physiological changes related to aging (in this case, decreased efficiency of ADRB2 signaling) when analyzing phenotypic effects of genetic variants.

摘要

先前的研究表明,β₂-肾上腺素能受体(ADRB2)的变体可能对肾上腺素能刺激的功能反应产生不同影响,从而可能调节心血管和代谢表型。我们检验了这样一个假设,即ADRB2的G/R16和Q/E27多态性或其单倍型可能调节普通人群的血压、心血管结构和功能或代谢性心血管危险因素。我们对普通人群进行了随机抽样(n = 571;年龄35至64岁)。在总体人群中,诊室血压和24小时动态血压均与ADRB2基因型无显著关联。心脏结构和功能也不受ADRB2多态性的影响。在对潜在混杂因素进行调整后,在较年轻人群(50岁以下)亚组中观察到R16等位基因与较高的收缩压相关。单倍型分析表明,较高的血压值更具体地与R16-Q27的存在相关。携带R16-Q27单倍型的较年轻人群还表现出心率降低、BMI升高、血糖降低和甘油三酯血症升高的趋势,这与对ADRB2刺激的心血管和代谢反应降低的遗传易感性假设一致。本研究没有提供ADRB2基因变异在血压调节中起主要作用的证据。然而,在ADRB2介导的活性出现与年龄相关的下降之前,可以在较年轻的受试者中观察到ADRB2多态性与心血管和代谢效应的关联。我们的研究强调,在分析基因变异的表型效应时,有必要考虑与衰老相关的(病理)生理变化(在这种情况下,ADRB2信号传导效率降低)。

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