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The Arg16Gly polymorphism of the β2-adrenergic receptor and the natriuretic response to rapid saline infusion in humans

机译：β2-肾上腺素能受体的Arg16Gly多态性与人对快速输注盐水的利钠盐反应

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The β2-adrenergic receptors (β2ARs) play a role in renal Na⁺ regulation. Subjects homozygous for glycine at amino acid 16 (Gly16) of the β2AR have been shown to have enhanced β2-mediated vascular relaxation when compared to subjects homozygous for arginine (Arg16). However, Gly16 subjects have been shown to have higher blood pressure than Arg16 subjects. Given the dominant role of the kidneys in long-term blood pressure regulation, we sought to determine whether there were differences in renal Na⁺ handling between Gly16 (n = 17) and Arg16 (n = 14) subjects (Gly16: age, 30 ± 2 years; body mass index (BMI), 25 ± 11 kg m⁻²; Arg16: age, 30 ± 2 years; BMI, 25 ± 1 kg m⁻²). We measured urinary Na⁺ content before and for 3 h following rapid intravenous saline infusion (30 ml kg⁻¹ in ∼16 min). Prior to the infusion, there were no differences in 24-h Na⁺ excretion between Gly16 and Arg16 subjects (Gly16, 183 ± 21 mmol; Arg16, 184 ± 20 mmol); however, systolic blood pressure (SBP) was significantly higher in Gly16 than Arg16 subjects with no differences observed in diastolic blood pressure (DBP) or mean arterial pressure (MAP) (SBP: Gly16, 117 ± 3 mmHg; Arg16, 109 ± 2 mmHg; DBP: Gly16, 78 ± 2 mmHg; Arg16, 77 ± 2 mmHg; MAP: Gly16, 90 ± 2 mmHg; Arg16, 89 ± 2 mmHg). With rapid saline infusion, MAP increased in both genotype groups (Gly16, 6.7%; Arg16, 3.4%; P > 0.05). In the 3 h following Na⁺ infusion, Na⁺ excretion was less in Gly16 when compared to Arg16 subjects, with a trend towards significance when expressed as total Na⁺ excreted (Gly16, 66 ± 7 mmol; Arg16, 85 ± 9 mmol; P = 0.07), and a significant difference when expressed as a fraction of the administered load (Gly16, 0.18 ± 0.02; Arg16, 0.28 ± 0.03; P < 0.01). These results suggest that the Arg16Gly polymorphism of the β2AR is associated with differences in natriuretic response to rapid saline infusion, which may influence long-term regulation of blood pressure.

机译：β2-肾上腺素能受体（β2ARs）在肾脏Na ^{+ 调节中起作用。与精氨酸纯合子（Arg16）相比，在β2AR的氨基酸16（Gly16）上纯合子的受试者显示出增强的β2介导的血管舒张作用。然而，已显示Gly16受试者比Arg16受试者具有更高的血压。考虑到肾脏在长期血压调节中的主要作用，我们试图确定在Gly16（n = 17）和Arg16（n = 14）受试者之间肾脏Na ^{+ 处理是否存在差异（Gly16：年龄，30±2岁；体重指数（BMI），25±11 kg m ^{−2 ； Arg16：年龄，30±2岁； BMI，25±1 kg m ^{−2 ）。我们在快速静脉滴注生理盐水（约16分钟后30 ml kg ^{-1 ）之前和之后的3小时内测量了尿Na ^{+ 的含量。输注前，Gly16和Arg16受试者之间的24小时Na ^{+ 排泄没有差异（Gly16，183±21 mmol； Arg16，184±20 mmol）； Gly16，Arg 16，184±20 mmol。然而，Gly16的收缩压（SBP）明显高于Arg16受试者，舒张压（DBP）或平均动脉压（MAP）均无差异（SBP：Gly16，117±3 mmHg; Arg16，109±2 mmHg ； DBP：Gly16，78±2 mmHg； Arg16，77±2 mmHg； MAP：Gly16，90±2 mmHg； Arg16，89±2 mmHg）。在快速输注盐水的情况下，两个基因型组的MAP均升高（Gly16，6.7％； Arg16，3.4％； P> 0.05）。在Na ^{+ 输注后的3小时内，与Arg16受试者相比，Gly16中的Na ^{+ 排泄较少，当以总Na ^{+表示时，有显着趋势排泄（Gly16，66±7 mmol； Arg16，85±9 mmol； P = 0.07），当表示为部分负荷时，差异显着（Gly16，0.18±0.02； Arg16，0.28±0.03 ; P <0.01）。这些结果表明，β2AR的Arg16Gly多态性与利钠对快速输注盐水反应的差异有关，这可能会影响血压的长期调节。}}}}}}}}}}

著录项

期刊名称 The Journal of Physiology
作者
Eric M Snyder; Stephen T Turner; Michael J Joyner; John H Eisenach; Bruce D Johnson;
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年(卷),期 2006(574),Pt 3
年度 2006
页码 947–954
总页数 8
原文格式 PDF
正文语种
中图分类神经科学;人体生理学;
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1. The Arg16Gly polymorphism of the beta2-adrenergic receptor and the natriuretic response to rapid saline infusion in humans. [J] . Snyder EM, Turner ST, Joyner MJ, The Journal of Physiology . 2006,第Pta3期

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2. The effect of antecedent hypoglycaemia on β2-adrenergic sensitivity in healthy participants with the Arg16Gly polymorphism of the β2-adrenergic receptor [J] . B. J. J. W. Schouwenberg, P. Smits, C. J. Tack, Diabetologia: clinical and experimental diabetes and metabolism . 2011,第5期

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3. Role of α2-Adrenergic Receptor Subtypes in the Acute Hypertensive Response to Hypertonic Saline Infusion in Anephric Mice [J] . Konstantinos P. Makaritsis, Conrado Johns, Irene Gavras, Hypertension: An Official Journal of the American Heart Association . 2000,第2期

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The Arg16Gly polymorphism of the β2-adrenergic receptor and the natriuretic response to rapid saline infusion in humans

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