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Relationship between urinary sodium excretion and serum aldosterone in patients with diabetes in the presence and absence of modifiers of the renin-angiotensin-aldosterone system

机译:存在和不存在肾素-血管紧张素-醛固酮系统调节剂的糖尿病患者尿钠排泄与血清醛固酮的关系

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摘要

Although low dietary salt intake has beneficial effects on BP (blood pressure), low 24hUNa (24 h urinary sodium excretion), the most accurate estimate of dietary salt intake, is associated with increased mortality in people with diabetes. In the non-diabetic population, low salt intake is associated with increased RAAS (renin-angiotensin-aldosterone system) activity. In this cross-sectional study, we examined the relationship between 24hUNa, PRA (plasma renin activity), serum aldosterone and BNP (brain natriuretic peptide) in patients with diabetes. Clinical characteristics, 24hUNa, PRA, serum aldosterone and BNP were recorded in 222 consecutive patients (77% with Type 2 diabetes) attending a diabetes clinic at a tertiary hospital. The relationship between 24hUNa, serum aldosterone, PRA, BNP, urinary potassium excretion, serum potassium, serum sodium, eGFR (estimated glomerular filtration rate), urinary albumin excretion and HbA1c (glycated haemoglobin) was examined by a multivariable regression model. Levels of 24hUNa significantly predicted serum aldosterone in a linear fashion (R2 =0.20, P=0.002). In the subgroup of patients (n=46) not taking RAAS-modifying agents, this relationship was also observed (R2 =0.10, P=0.03), and the effect of 24hUNa on serum aldosterone was found to be more pronounced than in the whole cohort (coefficient= -0.0014, compared with -0.0008). There was no demonstrable relationship between 24hUNa and PRA or BNP. Low 24hUNa is associated with increased serum aldosterone in people with diabetes, in the presence and absence of RAAS-modifying agents. This raises the possibility that stimulation of the RAAS may be a mechanism that contributes to adverse outcomes observed in patients with low 24hUNa.
机译:尽管低饮食盐摄入量对BP(血压)有有益作用,但低24hUNa(24 h尿钠排泄)是饮食盐摄入量的最准确估算,与糖尿病患者的死亡率增加有关。在非糖尿病人群中,低盐摄入与RAAS(肾素-血管紧张素-醛固酮系统)活性增加有关。在这项横断面研究中,我们检查了糖尿病患者中24hUNa,PRA(血浆肾素活性),血清醛固酮和BNP(脑利钠肽)之间的关系。临床特征,24hUNa,PRA,血清醛固酮和BNP在三级医院的一家糖尿病诊所就诊的222例连续患者(77%患有2型糖尿病)中被记录。通过多变量回归模型检查24hUNa,血清醛固酮,PRA,BNP,尿钾排泄,血清钾,血清钠,eGFR(估计的肾小球滤过率),尿白蛋白排泄和HbA1c(糖化血红蛋白)之间的关系。 24hUNa水平以线性方式显着预测血清醛固酮(R2 = 0.20,P = 0.002)。在未使用RAAS改良剂的患者亚组(n = 46)中,也观察到这种关系(R2 = 0.10,P = 0.03),并且发现24hUNa对血清醛固酮的作用比整个患者更明显队列(系数= -0.0014,而-0.0008)。 24hUNa与PRA或BNP之间无明显关系。在存在和不存在RAAS修饰剂的情况下,低24hUNa与糖尿病患者血清醛固酮水平升高有关。这增加了RAAS刺激可能是导致24hUNa低的患者不良预后的一种机制的可能性。

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