Clinical potential of eliglustat tartrate in the treatment of type 1 Gaucher disease

Research and reports in endocrine disorders Pub Date : 2014-05-14 DOI:10.2147/RRED.S36669

P. Kaplan

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引用次数: 1

Abstract

Nonneuropathic type 1 Gaucher disease is an autosomal recessive inherited disease caused by the deficiency or absence of beta glucocerebrosidase (beta glucosidase). The highest prevalence of type 1 is in Ashkenazi Jews, but it affects all ethnic groups. It manifests at any age but is seen predominantly in the first two decades. The phenotype is characterized by painless splenomegaly and secondary hypersplenism (low hemoglobin concentration and low platelet and white blood cell counts). Symptoms and signs include splenomegaly; chronic fatigue, frequent nose bleeds, prolonged bleeding, and/or bruising; hepatomegaly; bone pain, bone destruction and low bone density; and poor growth in childhood and delayed pubertal development. Current treatment with intravenous enzyme replacement has been generally successful. However, oral treatments have been developed because enzyme replacement is time-consuming and invasive, and intravenous infusions are not universally available for patients who live far from medical centers or home infusion nurses. Furthermore, it may become difficult to access veins after repeated infusions. Orally administered substrate reduction is a newer treatment approach. The aim is to limit the synthesis of the substrate, glucosylceramide. The residual intrinsic enzyme, acting alone or with recombinant enzyme, can then completely catabolize the smaller amounts of glucosylceramide that are transported into lysosomes. Eliglustat tartrate is a new specific inhibitor of glucosylceramide synthase. Phase III trials in humans have been completed. Eli- glustat tartrate has been shown to be efficacious and safe in adult humans. The results are as good or better compared with intravenous replacement with regard to reductions in spleen and liver enlargement and improvements in hemoglobin concentrations, platelet counts, and bone density, as well as decreases in biomarkers of Gaucher disease activity. Few adverse events, none of which was serious, have been reported. Eliglustat tartrate has the clinical potential to enable a larger number of patients with type 1 Gaucher disease to be treated successfully.

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酒石酸依格司他治疗1型戈谢病的临床潜力

非神经性1型戈谢病是一种常染色体隐性遗传疾病，由-葡萄糖脑苷酶(-葡萄糖苷酶)缺乏引起。1型患病率最高的是德系犹太人，但它影响所有种族。它表现在任何年龄，但主要出现在头20年。表型的特点是无痛性脾大和继发性脾功能亢进(低血红蛋白浓度和低血小板和白细胞计数)。症状和体征包括脾肿大;慢性疲劳、频繁流鼻血、长时间出血和/或瘀伤;肝肿大;骨痛、骨破坏、骨密度低;儿童期发育不良，青春期发育迟缓。目前静脉注射酶替代治疗总体上是成功的。然而，口服治疗已经发展起来，因为酶替代是耗时和侵入性的，静脉输注并不普遍适用于远离医疗中心或家庭输液护士的患者。此外，反复输注后可能难以进入静脉。口服底物还原是一种较新的治疗方法。目的是限制底物葡萄糖神经酰胺的合成。剩余的内在酶，单独或与重组酶一起作用，可以完全分解少量的葡萄糖神经酰胺，并将其转运到溶酶体中。酒石酸依利司他是一种新的葡萄糖神经酰胺合成酶特异性抑制剂。人体三期试验已经完成。酒石酸谷胱甘肽已被证明对成人有效且安全。在脾脏和肝脏肿大的减少、血红蛋白浓度、血小板计数和骨密度的改善以及戈谢病活动性生物标志物的降低方面，与静脉替代相比，结果同样好或更好。几乎没有不良事件的报道，没有一个是严重的。酒石酸Eliglustat具有临床潜力，可以使更多的1型戈谢病患者获得成功治疗。

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Research and reports in endocrine disorders

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