临床应用的新型矿皮质激素受体拮抗剂eplerenone

Nannan Wu, Yuanyuan Zhang, D. Zhao
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引用次数: 0

摘要

醛固酮是由肾上腺皮质的肾小球带产生的,是主要的矿物皮质激素。通过与盐皮质激素受体结合,调节钠和钾的吸收、分泌和滞留,从而维持稳定的血压水平。然而,醛固酮合成和代谢异常可能是致病的,并可能导致多器官纤维化和结构重塑。例如,高醛固酮血症与高血压、心力衰竭和肾脏疾病的发展密切相关。因此,可以对抗高浓度醛固酮的矿化皮质激素受体拮抗剂(MRAs)在治疗高醛固酮症引起的疾病中发挥重要作用。依普利酮作为一种新型的选择性MRA,与经典药物螺内酯相比,具有更好的治疗效果和更少的副作用。本文首先介绍醛固酮的生物合成和生物学特性,然后介绍高醛固酮血症如何促进某些疾病的进展。醛固酮是肾素-血管紧张素-醛固酮系统(RAAS)的重要组成部分,在原发性高血压、心房颤动和组织纤维化中起重要作用。其次,我们总结了目前依普利酮在控制原发性醛固酮增多症、高血压、心衰、肾病、胰岛素抵抗和肝损害方面的临床应用证据。令人兴奋的是,许多研究表明,在这些疾病中使用epleenone取得了良好的效果,并且出现了较少的不良反应,如高钾血症、代谢性酸中毒、低血压和急性肾衰竭,这表明epleenone是一种强效、安全的MRA和RAAS系统抑制剂。本文就依普利酮治疗一系列不同疾病的疗效及缺点作一综述。最终,我们希望阐明与高醛固酮血症相关疾病的未来治疗策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Eplerenone–A novel Mineralocorticoid receptor antagonist for the clinical application
Aldosterone is produced from the zona glomerulosa of the adrenal cortex in the adrenal gland, which is main mineralocorticoid hormone. Upon binding the mineralocorticoid receptor, it regulates sodium and potassium absorption, secretion, and retention, thereby maintaining stable blood pressure levels. However, abnormal aldosterone synthesis and metabolism could be pathogenic and contribute to multiple organ fibrosis and structural remodeling. For instance, hyperaldosteronemia is critically involved in the development of hypertension, heart failure (HF), and renal disease. Therefore, mineralocorticoid receptor antagonists (MRAs) that could fight against high concentrations of aldosterone play an important role in the treatment of diseases caused by hyperaldosteronism. Eplerenone, as a novel selective MRA, has better therapeutic efficiency and fewer side effects comparing to the classical drug spironolactone. In this review, first, we go through the biosynthesis and biologic properties of aldosterone and then introduce how hyperaldosteronemia facilitates certain diseases progression. Aldosterone is an important part of the renin-angiotensin-aldosterone system (RAAS), which plays a crucial role in essential hypertension, atrial tremor, and tissue fibrosis. Second, we summarize current evidence of clinical application of eplerenone in the control of primary aldosteronism, hypertension, HF, nephropathy, insulin resistance, and liver damage. It is exciting that many studies have shown that the use of eplerenone in these diseases yields good outcomes accompanied with fewer adverse effects such as hyperkalemia, metabolic acidosis, hypotension, and acute kidney failure, which indicates that eplerenone is a strong and safe MRA and inhibitor of RAAS system. This review focuses on therapeutic efficacy and disadvantages of eplerenone when treating a series of different diseases. Ultimately, we hope to shed light on future therapeutic strategies in diseases associated with hyperaldosteronemia.
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