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Enzyme therapy in Fabry disease: differential in vivo plasma clearance and metabolic effectiveness of plasma and splenic alpha-galactosidase A isozymes.

机译:法布里病的酶治疗:体内血浆清除率不同,血浆和脾脏的α-半乳糖苷酶A同工酶的代谢效率也不同。

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摘要

A pilot trial of enzyme replacement with splenic and plasma alpha-galactosidase A (alpha-D-galactosidase; alpha-D-galactoside galactohydrolase, EC 3.2.1.22) isozymes was undertaken in two brothers with Fabry disease, an X-linked glycosphingolipid storage disease. Six unentrapped doses (2000 units/kg) of each isozyme were administered intravenously to the respective recipients during a 117-day period. The circulating half-life of the splenic isozyme was about 10 min, whereas that for the plasma isozyme was approximately 70 min. No immune response was detected by skin and immunodiffusion tests or by alterations in the maximal activity or clearance kinetics for either isozyme after successive administrations. After each dose of the splenic isozyme, the concentration of the accumulated circulating substrate, trihexosylceramide (globotriaosylceramide), decreased maximally (approximately 50% of initial values) in 15 min and returned to preinfusion levels by 2-3 hr. In marked contrast, injection of the plasma isozyme decreased the circulating substrate levels 50-70% by 2-6 hr; the concentrations gradually returned to preinfusion values by 36-72 hr.
机译:在患有Fabry病(一种X连锁糖鞘脂贮积病)的两个兄弟中进行了用脾脏和血浆中的α-半乳糖苷酶A(α-D-半乳糖苷酶;α-D-半乳糖苷半乳糖水解酶,EC 3.2.1.22)同工酶替代酶的先导试验。 。在117天的期间内,分别向各自的接受者静脉内注射六种未包埋剂量(2000单位/千克)的每种同工酶。脾同工酶的循环半衰期约为10分钟,而血浆同工酶的循环半衰期约为70分钟。连续给药后,皮肤和免疫扩散试验或同工酶最大活性或清除动力学的改变均未检测到免疫反应。每次服用脾脏同工酶后,累积的循环底物三己糖基神经酰胺(globotriaosylceramide)的浓度在15分钟内最大降低(约为初始值的50%),并在2-3小时后恢复到输注前水平。形成鲜明对比的是,血浆同工酶的注射将循环底物水平降低了2-6小时,降低了50-70%的循环底物水平;浓度在36-72小时后逐渐恢复到输注前的水平。

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