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Rationale for treating oedema in Duchenne muscular dystrophy with eplerenone

机译:依普利酮治疗杜氏肌营养不良症水肿的基本原理

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摘要

Recently we reported a cytoplasmic sodium overload to cause a severe osmotic oedema in Duchenne muscular dystrophy (DMD). Our results suggested that this dual overload of sodium ions and water precedes the dystrophic process and persists until fatty muscle degeneration is complete. The present paper addresses the questions as to whether these overloads are important for the pathogenesis of the disease, and if so, whether they can be treated. As a first step, we investigated the effects of various diuretic drugs on a cell model of DMD, i.e. rat diaphragm strips previously exposed to amphotericin B. We found that both carbonic anhydrase inhibitors and aldosterone antagonists were able to repolarise depolarised muscle fibres. Since carbonic anhydrase inhibitors are known to have acidifying effects and this might be detrimental to the ventilation of DMD patients, we mainly concentrated on the modern spironolactone derivative, eplerenone. This drug had a very high repolarizing power, the parameter considered by us as being most relevant for a beneficial effect. In a pilot study we administered this drug to a 22-yr-old female DMD patient who was bound to an electric wheelchair and has had no corticosteroid therapy before. Eplerenone decreased both cytoplasmic sodium and water overload and increased muscle strength and mobility. We conclude that eplerenone has beneficial effects on DMD muscle. In our opinion the cytoplasmic oedema is cytotoxic and should be treated before fatty degeneration takes place.
机译:最近,我们报道了胞质钠超载导致杜兴氏肌营养不良症(DMD)的严重渗透性水肿。我们的结果表明,钠离子和水的这种双重超负荷先于营养不良过程,并一直持续到脂肪肌肉变性完全为止。本文讨论了有关这些超负荷对疾病的发病机理是否重要以及是否可以治疗的问题。第一步,我们研究了各种利尿药对DMD细胞模型(即先前暴露于两性霉素B的大鼠隔膜)的影响。我们发现碳酸酐酶抑制剂和醛固酮拮抗剂都能使去极化的肌纤维重新极化。由于已知碳酸酐酶抑制剂具有酸化作用,并且可能对DMD患者的通气有害,因此我们主要研究了现代螺内酯衍生物依普利农。该药物具有非常高的复极化能力,我们认为该参数与有益作用最相关。在一项先导研究中,我们向22岁的DDM女性患者服用了该药物,该患者被绑定到电动轮椅并且之前没有接受皮质类固醇治疗。依普利酮减少了细胞质钠和水的超负荷,并增加了肌肉的力量和活动能力。我们得出结论,依普利农对DMD肌肉具有有益作用。我们认为细胞质水肿具有细胞毒性,应在脂肪变性发生之前进行治疗。

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