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用酶抑制剂治疗戈谢病。

Treatment of Gaucher disease with an enzyme inhibitor.

作者信息

Radin N S

机构信息

Mental Health Research Institute, University of Michigan, Ann Arbor 48109-0676, USA.

出版信息

Glycoconj J. 1996 Apr;13(2):153-7. doi: 10.1007/BF00731489.

Abstract

The hypothesis is offered predicting that Gaucher patients could be treated with a drug that slows the synthesis of glucosylceramide, the lipid that accumulates in this disorder. The present therapeutic approach involves augmenting the defective enzyme, glucosylceramide beta-glucosidase, with exogenous beta-glucosidase isolated from human tissue. This spectacularly expensive mode of treatment should be replaceable with a suitable enzyme inhibitor that simply slows formation of the lipid and matches the rate of synthesis with the rate of the defective, slowly working beta-glucosidase. Several drugs that possess this ability are available, the best known of which is 1-phenyl-2-decanoylamino-3-morpholino-1-propanol (PDMP), a designer inhibitor that resembles the synthase's substrate and product. PDMP has been found to be effective in mice, rats, fish, and a wide variety of cultured cells. Its use, at suitable dosages, seems to be harmless, although long-term tests have not been made. The lack of suitable animal models of Gaucher disease has made it difficult to test the hypothesis adequately, but PDMP does rapidly lower the levels of glucosylceramide in normal animal tissues and the animals evidently do well with the lowered levels of glucosylceramide and its more complex glycolipid metabolites.

摘要

有人提出一种假说,预测戈谢病患者可以用一种能减缓葡糖神经酰胺合成的药物进行治疗,葡糖神经酰胺是在这种疾病中积累的脂质。目前的治疗方法是用人组织中分离出的外源性β-葡糖苷酶来增强有缺陷的酶——葡糖神经酰胺β-葡糖苷酶。这种极其昂贵的治疗方式应该可以被一种合适的酶抑制剂所取代,这种抑制剂只需减缓脂质的形成,并使合成速率与有缺陷的、工作缓慢的β-葡糖苷酶的速率相匹配。有几种具有这种能力的药物可供使用,其中最著名的是1-苯基-2-癸酰氨基-3-吗啉代-1-丙醇(PDMP),一种设计抑制剂,类似于合成酶的底物和产物。已发现PDMP在小鼠、大鼠、鱼类和多种培养细胞中有效。以适当剂量使用时,它似乎是无害的,不过尚未进行长期试验。由于缺乏合适的戈谢病动物模型,难以充分验证这一假说,但PDMP确实能迅速降低正常动物组织中葡糖神经酰胺的水平,而且动物在葡糖神经酰胺及其更复杂的糖脂代谢物水平降低的情况下显然状况良好。

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