Treatment with ataluren in four symptomatic Duchenne carriers. A pilot study.

Amir Dori, Marianna Scutifero, Luigia Passamano, Dario Zoppi, Lucia Ruggiero, Antonio Trabacca, Luisa Politano
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Abstract

Duchenne muscular dystrophy (DMD) is a devastating X-linked neuromuscular disorder caused by dystrophin gene deletions (75%), duplications (15-20%) and point mutations (5-10%), a small portion of which are nonsense mutations. Women carrying dystrophin gene mutations are commonly unaffected because the wild X allele may produce a sufficient amount of the dystrophin protein. However, approximately 8-10% of them may experience muscle symptoms and 50% of those over 40 years develop cardiomyopathy. The presence of symptoms defines the individual as an affected "symptomatic or manifesting carrier". Though there is no effective cure for DMD, therapies are available to slow the decline of muscle strength and delay the onset and progression of cardiac and respiratory impairment. These include ataluren for patients with nonsense mutations, and antisense oligonucleotides therapies, for patients with specific deletions. Symptomatic DMD female carriers are not included in these indications and little data documenting their management, often entrusted to the discretion of individual doctors, is present in the literature. In this article, we report the clinical and instrumental outcomes of four symptomatic DMD carriers, aged between 26 and 45 years, who were treated with ataluren for 21 to 73 months (average 47.3), and annually evaluated for muscle strength, respiratory and cardiological function. Two patients retain independent ambulation at ages 33 and 45, respectively. None of them developed respiratory involvement or cardiomyopathy. No clinical adverse effects or relevant abnormalities in routine laboratory values, were observed.

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对四名有症状的杜兴基因携带者进行阿塔卢仑治疗。试点研究。
杜氏肌营养不良症(DMD)是一种毁灭性的 X 连锁神经肌肉疾病,由肌营养不良基因缺失(75%)、重复(15-20%)和点突变(5-10%)引起,其中一小部分是无义突变。携带肌营养不良蛋白基因突变的女性通常不受影响,因为野生 X 等位基因可产生足量的肌营养不良蛋白。然而,其中约 8-10% 的人可能会出现肌肉症状,40 岁以上的患者中有 50% 会出现心肌病。出现症状的个体被定义为受影响的 "有症状或有表现的携带者"。虽然 DMD 尚无有效的治疗方法,但有一些疗法可减缓肌肉力量的下降,并延缓心脏和呼吸功能损害的发生和发展。这些疗法包括针对无义突变患者的阿塔卢仁疗法和针对特定缺失患者的反义寡核苷酸疗法。有症状的 DMD 女性携带者并不包括在这些适应症中,文献中也几乎没有记录她们的治疗数据,她们的治疗通常由医生自行决定。在本文中,我们报告了四名有症状的 DMD 携带者的临床和器械治疗结果,她们的年龄在 26 岁至 45 岁之间,接受了 21 个月至 73 个月(平均 47.3 个月)的阿达仑治疗,并每年接受一次肌力、呼吸和心脏功能评估。两名患者分别在 33 岁和 45 岁时仍能独立行走。他们均未出现呼吸系统受累或心肌病变。没有观察到任何临床不良反应或常规实验室数值的相关异常。
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