The Arg389Gly beta1-adrenoceptor gene polymorphism determines contractile response to catecholamines.

Karl La Rosée, Michael Huntgeburth, Stephan Rosenkranz, Michael Böhm, Petra Schnabel
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引用次数: 65

Abstract

Objectives: Recently, the Arg389Gly beta1-adrenoceptor (beta1AR) gene polymorphism has been detected. The Arg variant exhibited increased responsiveness to agonist-induced stimulation in vitro. Functional studies in isolated human atrial muscle strips and in-vivo studies revealed contradictory results regarding the functional relevance of this polymorphism. We sought to characterize the functional consequences of the Arg389Gly beta1-AR polymorphism in 30 consecutive healthy male volunteers in vivo.

Methods: beta1-AR genotype was determined by PCR and restriction analysis, which was confirmed by DNA sequencing. We compared heart rate, blood pressure, and contractile response of the various genotype carriers with a modified dobutamine stress echocardiography protocol.

Results: Subjects homozygous for the Arg389 beta1AR showed a significantly higher increase in fractional shortening upon cumulative doses of dobutamine as compared to subjects carrying one or two copies of the Gly389 allele. A statistically significant difference was observed at a dobutamine dose of 10 microg/kg/min (46.5 +/- 1.3 vs. 41.8 +/- 1.0 %; P = 0.023) and was maximal at 40 microg/kg/min (61.9 +/- 1.4 vs. 52.8 +/- 1.6; P = 0.001). As a result, the systolic blood pressure response to dobutamine was significantly enhanced in individuals homozygous for the Arg389 allele, whereas the effect on heart rate did not differ between the two groups. Normalization for changing afterload conditions by calculating the pressure-dimension ratio revealed similar effects, indicating that the beta1AR-mediated effects are mainly a result of increased myocardial inotropy.

Conclusion: These data indicate that the Arg389Gly beta1AR polymorphism is functionally relevant in vivo and determines contractile responsiveness to catecholamines in humans.

Arg389Gly - β -肾上腺素受体基因多态性决定了对儿茶酚胺的收缩反应。
目的:近年来,人们检测到Arg389Gly β -肾上腺素受体(beta1AR)基因多态性。Arg变体在体外对激动剂诱导的刺激表现出更高的反应性。分离的人类心房肌条的功能研究和体内研究揭示了关于这种多态性的功能相关性的矛盾结果。我们试图在30名连续的健康男性志愿者体内描述Arg389Gly β 1- ar多态性的功能后果。方法:采用PCR和限制性内切分析方法测定β 1- ar基因型,并进行DNA测序。我们用改良的多巴酚丁胺应激超声心动图方案比较了不同基因型携带者的心率、血压和收缩反应。结果:与携带一个或两个Gly389等位基因拷贝的受试者相比,Arg389 β 1ar纯合子的受试者在累积剂量多巴酚丁胺的作用下显着增加了分数缩短。多巴酚丁胺剂量为10 μ g/kg/min时,差异有统计学意义(46.5 +/- 1.3 vs 41.8 +/- 1.0%;P = 0.023),在40 μ g/kg/min时最大(61.9 +/- 1.4 vs. 52.8 +/- 1.6;P = 0.001)。结果,在Arg389等位基因纯合的个体中,多巴酚丁胺对收缩压的反应显著增强,而对心率的影响在两组之间没有差异。通过计算压力-尺寸比对改变后负荷条件进行归一化也显示出类似的效应,表明β - 1ar介导的效应主要是心肌肌力增强的结果。结论:这些数据表明Arg389Gly β 1ar多态性在体内具有功能相关性,并决定了人类对儿茶酚胺的收缩反应性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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