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A Patient with Bilateral Primary Aldosteronism Refractory to Oral Eplerenone Who Responded to Esaxerenone with Increased Renin Activity

机译:口服依普利酮难治的双侧原发性醛固酮增多症患者对肾上腺素活动增强的依沙酮酮有反应

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Objective: Adverse events of drug therapyBackground: When mineralocorticoid receptor antagonist therapy is initiated for primary aldosteronism, the response of plas-ma renin activity indicates the level of cardiovascular risk. The purpose of this article was to compare the effect of mineralocorticoid receptor blockers on plasma renin activity levels in a patient with primary aldosteronism.Case Report: The patient was a 45-year-old male with severe hypertension. Because his aldosterone/renin ratio was high and a saline infusion test was positive, primary aldosteronism was diagnosed. Computed tomography revealed a low-density mass measuring 10 mm in the left adrenal gland. Segmental adrenal vein sampling demonstrated bilateral primary aldosteronism, so pharmacotherapy was started. Before treatment, his plasma renin activity was 0.5 ng/mL/hour. Eplerenone was commenced and the dose was increased to 100 mg/day. However, his plasma renin activity was still 0.8 ng/mL/hour and the maximum dose of eplerenone did not elevate plasma re-nin activity above 1 ng/mL/hour. Since plasma renin activity remained below 1 ng/mL/hour with mineralocorti-coid receptor antagonist therapy, this patient was considered to have a higher cardiovascular risk than patients with essential hypertension. Accordingly, eplerenone was switched to esaxerenone, a new generation mineralo-corticoid receptor blocker that became available in May 2019. After switching to esaxerenone (5 mg/day), the patient’s plasma renin activity increased to 1.8 ng/mL/hour and subsequently remained at 1 ng/mL/hour or higher.Conclusions: This is the first case report to present interesting changes of plasma renin activity in a primary aldosteronism patient after switching from eplerenone to esaxerenone. Elevation of plasma renin activity by esaxerenone in our primary aldosteronism patient reflected a mineralocorticoid receptor antagonistic effect that may have al-leviated excessive mineralocorticoid receptor activation and volume expansion.
机译:目的:药物治疗的不良事件背景:开始针对原发性醛固酮增多症的盐皮质激素受体拮抗剂治疗时,血浆肾素活性的反应表明存在心血管风险。本文旨在比较盐皮质激素受体阻滞剂对原发性醛固酮增多症患者血浆肾素活性水平的影响。病例报告:该患者是一名45岁的男性,患有严重的高血压。由于他的醛固酮/肾素比率高且盐水注入试验呈阳性,因此诊断出原发性醛固酮增多症。计算机断层扫描显示左肾上腺的低密度肿块为10 mm。肾上腺节段采样显示双侧原发性醛固酮增多症,因此开始了药物治疗。治疗前,他的血浆肾素活性为0.5 ng / mL /小时。开始使用依普利农,剂量增加至100 mg / day。但是,他的血浆肾素活性仍为0.8 ng / mL /小时,依匹乐酮的最大剂量并未将血浆肾素活性提高至1 ng / mL /小时以上。由于用矿物质皮质激素受体拮抗剂治疗血浆肾素活性仍低于1 ng / mL /小时,因此该患者被认为比原发性高血压患者有更高的心血管风险。因此,依普利农转用依沙酮烯酮,一种新一代的盐皮质激素受体阻滞剂,于2019年5月上市。转用依沙酮烯酮(5毫克/天)后,患者的血浆肾素活性增至1.8 ng / mL /小时,随后保持不变结论:这是第一例在原发性醛固酮增多症患者从依普利农转为依沙酮酮后血浆肾素活性发生有趣变化的病例报告。在我们的原发性醛固酮增多症患者中,依沙酮烯酮引起的血浆肾素活性升高反映了盐皮质激素受体拮抗作用,可能消除了过多的盐皮质激素受体活化和体积扩张。

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