鞘糖脂合成抑制剂的设计与临床开发:发明会成为需求之母吗?
The design and clinical development of inhibitors of glycosphingolipid synthesis: will invention be the mother of necessity?
作者信息
Shayman James A
机构信息
Department of Internal Medicine, University of Michigan, 1150 West Medical Center Dr, Ann Arbor, MI 48109-5676, USA.
出版信息
Trans Am Clin Climatol Assoc. 2013;124:46-60.
Abstract
The treatment of glycosphingolipid storage diseases by synthesis inhibition was first proposed 40 years ago as an alternative approach to enzyme replacement therapy. We have pursued this strategy through the rational design of potent and selective inhibitors of glucosylceramide synthase, the first step in glycosphingolipid synthesis. Eliglustat tartrate was the result of these efforts and is currently the focus of phase 3 trials for type 1 Gaucher disease. Phase 2 studies showed a reduction in splenomegaly and hepatomegaly and improvements of anemia and thrombocytopenia at levels equivalent to or exceeding the historic response to imiglucerase. Structural analogues of eliglustat have also been designed that lack pgp-1 recognition and cross the blood brain barrier. These may have utility for central nervous system- based sphingolipidoses. Because glycosphingolipids are important regulators of receptor tyrosine kinases, glucosylceramide synthase inhibitors may also be beneficial for disorders such as type 2 diabetes mellitus and polycystic kidney disease.
摘要
40年前首次提出通过合成抑制来治疗糖鞘脂贮积病,作为酶替代疗法的一种替代方法。我们通过合理设计强效且选择性的葡糖神经酰胺合酶抑制剂来推行这一策略,葡糖神经酰胺合酶是糖鞘脂合成的第一步。酒石酸依格列斯他就是这些努力的成果,目前是1型戈谢病3期试验的重点。2期研究表明,脾肿大和肝肿大有所减轻,贫血和血小板减少症有所改善,改善程度等同于或超过了历史上对伊米苷酶的反应。还设计了缺乏pgp - 1识别且能穿过血脑屏障的依格列斯他结构类似物。这些类似物可能对基于中枢神经系统的鞘脂类疾病有用。由于糖鞘脂是受体酪氨酸激酶的重要调节剂,葡糖神经酰胺合酶抑制剂可能对2型糖尿病和多囊肾病等疾病也有益处。
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