Tylicki Leszek, Rutkowski Przemysław, Renke Marcin, Larczyński Wojciech, Aleksandrowicz Ewa, Lysiak-Szydlowska Wiesława, Rutkowski Bolesław
Department of Nephrology Transplantology and Internal Medicine, Medical University of Gdansk, Gdansk, Poland.
Am J Kidney Dis. 2008 Sep;52(3):486-93. doi: 10.1053/j.ajkd.2008.02.297. Epub 2008 Apr 18.
Agents inhibiting the renin-angiotensin-aldosterone (RAAS) system have an important role in slowing the progression of chronic kidney disease. We evaluated the hypothesis that the addition of an aldosterone receptor antagonist to an angiotensin-converting enzyme (ACE) inhibitor and angiotensin II type 1 (AT-1) receptor blocker (ARB) (triple RAAS blockade) may provide an additional benefit compared with an ACE inhibitor and ARB (double RAAS blockade).
Randomized open controlled crossover study.
SETTING & PARTICIPANTS: 18 whites (7 women, 11 men) from the Outpatient Department of Nephrology with chronic nondiabetic proteinuric kidney diseases, mean age 42.4 +/- 1.9 years (SEM).
In the 8-week run-in period, all participants received the ACE inhibitor cilazapril (5 mg), the ARB telmisartan (80 mg), and the diuretic hydrochlorothiazide (12.5 mg) as double RAAS blockade to achieve the target blood pressure of less than 130/80 mm Hg. Participants were then randomly assigned to 2 treatment sequences, either the addition of spironolactone (25 mg) (triple RAAS blockade) through 8 weeks followed by double RAAS blockade through 8 weeks (sequence 1) or double RAAS blockade followed by triple RAAS blockade (sequence 2).
24-hour urine protein excretion (primary end point) and markers of tubular injury and fibrosis (secondary end points). Analysis was performed using analysis of variance for repeated measurements.
At baseline, mean serum creatinine level was 1.16 +/- 0.09 mg/dL (103 +/- 8 micromol/L), estimated glomerular filtration rate was 107.8 mL/min (95% confidence interval, 93 to 140.9 [1.8 mL/s; 95% confidence interval, 1.55 to 2.35; Cockcroft-Gault formula), and 24-hour mean proteinuria was 0.97 +/- 0.18 g. Mean urine protein excretion was 0.7 g/24 h (95% confidence interval, 0.48 to 0.92) less after triple RAAS blockade than after double RAAS blockade (P = 0.01), without change in blood pressure. Urine excretion of N-acetyl-beta-d-glucosaminidase (P = 0.02) and amino-terminal propeptide of type III procollagen (P = 0.05) also significantly decreased. Potassium levels increased significantly after triple therapy (P = 0.02). However, no patient was withdrawn because of adverse effects.
Absence of blinding, small sample size, short treatment period, absence of histological assessment.
Administration of an aldosterone receptor antagonist in addition to double RAAS blockade with an ACE inhibitor and ARB may slow the progression of chronic kidney disease. Additional studies are necessary to confirm this result.
抑制肾素 - 血管紧张素 - 醛固酮系统(RAAS)的药物在减缓慢性肾病进展中起重要作用。我们评估了这样一种假设,即与血管紧张素转换酶(ACE)抑制剂和血管紧张素II 1型(AT - 1)受体阻滞剂(双重RAAS阻断)相比,在ACE抑制剂和ARB基础上加用醛固酮受体拮抗剂(三重RAAS阻断)可能带来额外益处。
随机开放对照交叉研究。
来自肾病门诊的18名白人(7名女性,11名男性),患有慢性非糖尿病性蛋白尿肾病,平均年龄42.4±1.9岁(标准误)。
在8周的导入期,所有参与者接受ACE抑制剂西拉普利(5毫克)、ARB替米沙坦(80毫克)和利尿剂氢氯噻嗪(12.5毫克)作为双重RAAS阻断治疗,以达到血压低于130/80毫米汞柱的目标。然后参与者被随机分配到2种治疗顺序,要么先加用螺内酯(25毫克)进行8周的三重RAAS阻断,随后进行8周的双重RAAS阻断(顺序1),要么先进行双重RAAS阻断,然后进行三重RAAS阻断(顺序2)。
24小时尿蛋白排泄(主要终点)以及肾小管损伤和纤维化标志物(次要终点)。使用重复测量方差分析进行分析。
基线时,平均血清肌酐水平为1.16±0.09毫克/分升(103±8微摩尔/升),估计肾小球滤过率为107.8毫升/分钟(95%置信区间,93至140.9[1.8毫升/秒;95%置信区间,1.55至2.35;Cockcroft - Gault公式]),24小时平均蛋白尿为0.97±0.18克。与双重RAAS阻断后相比,三重RAAS阻断后平均尿蛋白排泄量少0.7克/24小时(95%置信区间,0.48至0.92)(P = 0.01),血压无变化。N - 乙酰 - β - D - 氨基葡萄糖苷酶的尿排泄量(P = 0.02)和III型前胶原氨基端前肽(P = 0.05)也显著降低。三重治疗后血钾水平显著升高(P = 0.02)。然而,没有患者因不良反应退出研究。
缺乏盲法、样本量小、治疗期短、缺乏组织学评估。
在使用ACE抑制剂和ARB进行双重RAAS阻断的基础上加用醛固酮受体拮抗剂可能减缓慢性肾病的进展。需要进一步研究来证实这一结果。
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