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New therapies in the management of Niemann-Pick type C disease: clinical utility of miglustat

机译:Niemann-Pick C型疾病管理的新疗法:米格司他的临床应用

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Niemann-Pick disease type C (NP-C) is an autosomal recessive disorder characterized by progressive neurological deterioration leading to premature death. The disease is caused by mutations in one of two genes, NPC1 or NPC2 , leading to impaired intracellular lipid transport and build-up of lipids in various tissues, particularly the brain. Miglustat (Zavesca?), a reversible inhibitor of glycosphingolipid synthesis, has recently been authorized in the European Union, Brazil and South Korea for the treatment of progressive neurological symptoms in adult and pediatric patients, and represents the first specific treatment for NP-C. Here we review current data on the pharmacology, efficacy, safety and tolerability of miglustat in patients with NP-C, based on findings from a prospective clinical trial, preclinical and retrospective studies, and case reports. Findings demonstrated clinically relevant beneficial effects of miglustat on neurological disease progression in adult, juvenile and pediatric patients with NP-C, particularly those diagnosed in late childhood (6–11 years) and in juveniles and adults (12 years and older), compared with those diagnosed in early childhood (younger than 6 years). Miglustat therapy was well-tolerated in all age groups. With the approval of miglustat, treatment of patients with NP-C can now be aimed toward stabilizing neurological disease, which is likely the best attainable therapeutic goal for this disorder.
机译:C型尼曼-皮克病(NP-C)是一种常染色体隐性遗传疾病,其特征是进行性神经功能恶化导致过早死亡。该疾病是由两个基因之一NPC1或NPC2的突变引起的,导致细胞内脂质运输受损以及各种组织(尤其是大脑)中脂质的积累。 Miglustat(Zavesca ?)是糖鞘脂合成的可逆抑制剂,最近已在欧盟,巴西和韩国获得批准,可用于治疗成人和儿科患者的进行性神经系统症状,并且是第一个NP-C的特定治疗。在这里,我们根据前瞻性临床试验,临床前和回顾性研究的结果以及病例报告,回顾了NP-C患者使用miglustat的药理学,功效,安全性和耐受性的最新数据。研究结果表明,米格司他对成人,少年和小儿NP-C患者,特别是在儿童晚期(6-11岁),少年和成人(12岁及以上)诊断的神经系统疾病进展具有临床相关的有益作用。那些在儿童早期(小于6岁)被诊断出的人。在所有年龄段,Miglustat治疗均耐受良好。通过米格司他的批准,NP-C患者的治疗现在可以针对稳定神经系统疾病,这可能是该疾病可达到的最佳治疗目标。

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