依普利酮单药长期治疗原发性高血压的降压效果:基线尿钠排泄与降压效果的关系。
Antihypertensive Effect of Long-Term Monotherapy with Esaxerenone in Patients with Essential Hypertension: Relationship Between Baseline Urinary Sodium Excretion and Its Antihypertensive Effect.
机构信息
Cardiovascular Hospital of Central Japan, Shimohakoda 740, Hokkitsumachi, Shibukawa, Gunma, 377-0061, Japan.
Daiichi Sankyo Co., Ltd., Tokyo, Japan.
出版信息
Adv Ther. 2022 Oct;39(10):4779-4791. doi: 10.1007/s12325-022-02282-3. Epub 2022 Aug 17.
INTRODUCTION
The blood pressure (BP) control mechanism for mineralocorticoid receptor blockers is unclear, and analysis of their use as a single agent in the clinical setting is required to resolve this uncertainty. There is a paucity of data on esaxerenone monotherapy assessing its long-term antihypertensive effect and urinary biomarkers.
METHODS
This post hoc exploratory substudy of a long-term phase 3 study evaluated the effect of esaxerenone monotherapy (2.5 or 5 mg/day) in treatment-naïve patients who continued the therapy during the 52-week study period (n = 25). In addition to blood biomarkers, urinary biomarkers were also assessed in 24-h urine collection samples.
RESULTS
Esaxerenone monotherapy was associated with consistent reductions in systolic/diastolic BP in the substudy population (- 23.5/- 13.1 mmHg at week 52, p < 0.001 vs baseline). Plasma aldosterone concentrations and plasma renin activity significantly increased during esaxerenone monotherapy at all time points. On the basis of the observations that both urine volume and urinary sodium excretion also decreased up to the end of the study, and were significantly lower at 12 weeks, patients were further categorized into higher/lower urinary sodium excretion subgroups according to whether their baseline values were above or below the median. In the group with higher baseline urinary sodium excretion, esaxerenone exhibited a significantly greater decrease in systolic/diastolic BP compared to the lower baseline group.
CONCLUSION
Esaxerenone exhibited sustained and stable antihypertensive activity even when administered as a single agent for 52 weeks in patients with essential hypertension. The additional urinary biomarker analysis suggests that the BP-lowering effects of esaxerenone may be partly exerted via mechanisms related to salt and water retention, and that the effect is particularly pronounced in patients with hypertension and higher baseline urinary sodium excretion, which may reflect a state of excessive salt intake.
TRIAL REGISTRATION
NCT02722265.
简介
醛固酮受体阻滞剂的血压(BP)控制机制尚不清楚,需要分析其在临床环境中作为单一药物的使用情况,以解决这一不确定性。目前关于依普利酮单药治疗的长期降压效果和尿生物标志物的数据很少。
方法
本研究是一项长期 3 期研究的事后探索性亚研究,评估了依普利酮单药治疗(2.5 或 5mg/天)在治疗初治患者中的效果,这些患者在研究期间(n=25)继续接受治疗52 周。除了血液生物标志物外,还在 24 小时尿液采集样本中评估了尿生物标志物。
结果
依普利酮单药治疗与研究亚组人群的收缩压/舒张压持续降低相关(第 52 周时为-23.5/-13.1mmHg,p<0.001 与基线相比)。在依普利酮单药治疗的所有时间点,血浆醛固酮浓度和血浆肾素活性均显著升高。基于观察到直至研究结束时尿液量和尿钠排泄也减少,并且在 12 周时显著降低的结果,根据基线值是否高于或低于中位数,患者进一步分为尿钠排泄较高/较低亚组。在基线尿钠排泄较高的组中,与基线较低的组相比,依普利酮的收缩压/舒张压降低幅度明显更大。
结论
在原发性高血压患者中,依普利酮作为单一药物治疗 52 周时,表现出持续稳定的降压活性。额外的尿生物标志物分析表明,依普利酮的降压作用可能部分通过与盐和水潴留相关的机制发挥作用,并且在高血压和基线尿钠排泄较高的患者中作用更为明显,这可能反映了过度盐摄入的状态。
试验注册
NCT02722265。
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