帕替罗默对正在服用和未服用RAAS抑制剂的高钾血症患者的影响。
Effect of Patiromer in Hyperkalemic Patients Taking and Not Taking RAAS Inhibitors.
作者信息
Kloner Robert A, Gross Coleman, Yuan Jinwei, Conrad Ansgar, Pergola Pablo E
机构信息
1 Huntington Medical Research Institutes, Pasadena, CA, USA.
2 Division of Cardiovascular Medicine, Department of Medicine, Keck School of Medicine of University of Southern California, Los Angeles, CA, USA.
出版信息
J Cardiovasc Pharmacol Ther. 2018 Nov;23(6):524-531. doi: 10.1177/1074248418788334. Epub 2018 Aug 14.
INTRODUCTION
Hyperkalemia (potassium >5.0 mEq/L) affects heart failure patients with renal disease regardless of the use of renin-angiotensin-aldosterone system inhibitors (RAASi). The open-label TOURMALINE study showed that patiromer, a sodium-free, nonabsorbed potassium binder, lowers serum potassium of hyperkalemic patients similarly when given with or without food; unlike prior studies, patients were not required to be taking RAASi. We conducted post hoc analyses to provide the first report of patiromer in patients not taking RAASi.
METHODS
Hyperkalemic patients received patiromer, 8.4 g/d to start, adjusted to achieve and maintain serum potassium of 3.8 to 5.0 mEq/L. If taking RAASi, stable doses were required. The primary end point was the proportion of patients with serum potassium 3.8 to 5.0 mEq/L at week 3 or 4. This analysis presents data by patients taking or not taking RAASi.
RESULTS
Demographics and baseline characteristics were similar in patients taking (n = 67) and not taking RAASi (n = 45). Baseline mean (SD) serum potassium was 5.37 (0.37) mEq/L and 5.42 (0.43) mEq/L in patients taking and not taking RAASi, respectively. Mean (SD) daily patiromer doses were similar (10.7 [3.2] and 11.5 [4.0] g, respectively). The primary end point was achieved in 85% (95% confidence interval [CI]: 74-93) of patients taking RAASi and in 84% (95% CI: 71-94) of patients not taking RAASi. From baseline to week 4, the mean (SE) change in serum potassium was -0.67 (0.08) mEq/L in patients taking RAASi and -0.56 (0.10) mEq/L in patients not taking RAASi (both P < .0001 vs baseline, P = nonsignificant between groups). Adverse events were reported in 26 (39%) patients taking RAASi and 25 (54%) not taking RAASi; the most common adverse event was diarrhea (2% and 11%, respectively; no cases were severe). Five patients (2 taking RAASi) reported 6 serious adverse events; none considered related to patiromer.
CONCLUSIONS
Patiromer was effective and generally well-tolerated for hyperkalemia treatment, whether or not patients were taking RAAS inhibitors.
引言
高钾血症(血钾>5.0 mEq/L)会影响患有肾脏疾病的心力衰竭患者,无论是否使用肾素-血管紧张素-醛固酮系统抑制剂(RAASi)。开放标签的TOURMALINE研究表明,帕替罗姆是一种无钠、不被吸收的钾结合剂,无论与食物同服与否,降低高钾血症患者血清钾的效果相似;与既往研究不同的是,患者无需服用RAASi。我们进行了事后分析,以首次报告帕替罗姆在未服用RAASi患者中的情况。
方法
高钾血症患者起始服用帕替罗姆8.4 g/d,并进行调整以达到并维持血清钾在3.8至5.0 mEq/L。如果正在服用RAASi,则需要稳定剂量。主要终点是第3周或第4周时血清钾在3.8至5.0 mEq/L的患者比例。本分析按是否服用RAASi呈现数据。
结果
服用RAASi的患者(n = 67)和未服用RAASi的患者(n = 45)的人口统计学和基线特征相似。服用和未服用RAASi的患者基线平均(标准差)血清钾分别为5.37(0.37)mEq/L和5.42(0.43)mEq/L。平均(标准差)每日帕替罗姆剂量相似(分别为10.7 [3.2] g和11.5 [4.0] g)。服用RAASi的患者中有85%(95%置信区间[CI]:74 - 93)达到主要终点,未服用RAASi的患者中有84%(95% CI:71 - 94)达到主要终点。从基线到第4周,服用RAASi的患者血清钾平均(标准误)变化为 -0.67(0.08)mEq/L,未服用RAASi的患者为 -0.56(0.10)mEq/L(两组与基线相比P均<0.0001,组间P无显著性差异)。服用RAASi的患者中有26例(39%)报告了不良事件,未服用RAASi的患者中有25例(54%)报告了不良事件;最常见的不良事件是腹泻(分别为2%和11%;均无严重病例)。5例患者(2例服用RAASi)报告了6例严重不良事件;均认为与帕替罗姆无关。
结论
无论患者是否服用RAAS抑制剂,帕替罗姆治疗高钾血症均有效且耐受性良好。
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