帕替罗姆、环硅酸锆钠和聚苯乙烯磺酸钠治疗高钾血症的临床效用:一项循证综述
Clinical utility of patiromer, sodium zirconium cyclosilicate, and sodium polystyrene sulfonate for the treatment of hyperkalemia: an evidence-based review.
作者信息
Beccari Mario V, Meaney Calvin J
机构信息
Department of Pharmacy Practice, School of Pharmacy and Pharmaceutical Sciences, University at Buffalo, Buffalo, NY, USA.
出版信息
Core Evid. 2017 Mar 23;12:11-24. doi: 10.2147/CE.S129555. eCollection 2017.
INTRODUCTION
Hyperkalemia is a serious medical condition that often manifests in patients with chronic kidney disease and heart failure. Renin-angiotensin-aldosterone system inhibitors are known to improve outcomes in these disease states but can also cause drug-induced hyperkalemia. New therapeutic options exist for managing hyperkalemia in these patients which warrant evidence-based evaluation.
AIM
The objective of this article was to review the efficacy and safety evidence for patiromer, sodium zirconium cyclosilicate (ZS9), and sodium polystyrene sulfonate (SPS) for the treatment of hyperkalemia.
EVIDENCE REVIEW
Current treatment options to enhance potassium excretion are SPS and loop diuretics, which are complicated by ambiguous efficacy and known toxicities. Patiromer and ZS9 are new agents designed to address this treatment gap. Both unabsorbable compounds bind potassium in the gastrointestinal (GI) tract to facilitate fecal excretion. The capacity to bind other medications in the GI tract infers high drug-drug interaction potential, which has been demonstrated with patiromer but not yet investigated with ZS9 or SPS. Phase II and III clinical trials of patiromer and ZS9 demonstrated clear evidence of a dose-dependent potassium-lowering effect and the ability to initiate, maintain, or titrate renin-angiotensin-aldosterone system inhibitors. There is limited evidence base for SPS: two small clinical trials indicated potassium reduction in chronic hyperkalemia. All agents may cause adverse GI effects, although they are less frequent with ZS9. Concerns remain for SPS to cause rare GI damage. Electrolyte abnormalities occurred with patiromer and SPS, whereas urinary tract infections, edema, and corrected QT-interval prolongations were reported with ZS9.
CONCLUSION
Patiromer and ZS9 have improved upon the age-old standard SPS for the treatment of hyperkalemia. Additional research should focus on drug-drug interactions in patients on multiple medications, incidence of rare adverse events, and use in high-risk populations.
引言
高钾血症是一种严重的医学病症,常出现在慢性肾病和心力衰竭患者中。已知肾素 - 血管紧张素 - 醛固酮系统抑制剂可改善这些疾病状态下的预后,但也可导致药物性高钾血症。对于管理这些患者的高钾血症,存在新的治疗选择,这需要进行循证评估。
目的
本文的目的是综述帕替罗姆、环硅锆酸钠(ZS9)和聚苯乙烯磺酸钠(SPS)治疗高钾血症的疗效和安全性证据。
证据综述
目前用于促进钾排泄的治疗选择是SPS和襻利尿剂,其疗效不明确且存在已知毒性,情况较为复杂。帕替罗姆和ZS9是旨在填补这一治疗空白的新型药物。这两种不可吸收的化合物在胃肠道(GI)中结合钾,以促进粪便排泄。在胃肠道中结合其他药物的能力意味着具有较高的药物相互作用潜力,这在帕替罗姆中已得到证实,但ZS9或SPS尚未进行研究。帕替罗姆和ZS9的II期和III期临床试验证明了剂量依赖性降钾作用以及启动、维持或滴定肾素 - 血管紧张素 - 醛固酮系统抑制剂的能力的明确证据。SPS的证据基础有限:两项小型临床试验表明可降低慢性高钾血症患者的血钾水平。所有药物都可能引起胃肠道不良反应,不过ZS9引起的频率较低。对于SPS导致罕见胃肠道损伤的担忧依然存在。帕替罗姆和SPS出现了电解质异常,而ZS9报告有尿路感染、水肿和校正QT间期延长。
结论
在治疗高钾血症方面,帕替罗姆和ZS9相较于古老的标准药物SPS有了改进。进一步的研究应聚焦于服用多种药物患者的药物相互作用、罕见不良事件的发生率以及在高危人群中的应用。
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