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Modification of aspartoacylase for potential use in enzyme replacement therapy for the treatment of Canavan disease.

机译:修饰天冬氨酸酰化酶,可潜在地用于治疗Canavan病的酶替代疗法中。

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Canavan disease is a fatal neurological disease without any effective treatments to slow the relentless progress of this disorder. Enzyme replacement therapy has been used effectively to treat a number of metabolic disorders, but the presence of the blood-brain-barrier presents an additional challenge in the treatment of neurological disorders. Studies have begun with the aim of establishing a treatment protocol that can effectively replace the defective enzyme in Canavan disease patients. The human enzyme, aspartoacylase, has been cloned, expressed and purified, and the surface lysyl groups modified through PEGylation. Fully active modified enzymes were administered to mice that are defective in this enzyme and that show many of the symptoms of Canavan disease. Statistically significant increases in brain enzyme activity levels have been achieved in this animal model, as well as decreases in the elevated substrate levels that mimic those found in Canavan disease patients. These results demonstrate that the modified enzyme is gaining access to the brain and functions to correct this metabolic defect. The stage is now set for a long term study to optimize this enzyme replacement approach for the development of a treatment protocol.
机译:卡纳万病是一种致命的神经系统疾病,没有任何有效的治疗方法来减缓这种疾病的持续发展。酶替代疗法已被有效地用于治疗许多代谢性疾病,但是血脑屏障的存在对神经系统疾病的治疗提出了另外的挑战。为了建立可有效替代Canavan病患者中缺陷酶的治疗方案,研究已经开始。已经克隆,表达和纯化了人类酶天冬酰化酶,并通过PEG化修饰了表面赖氨酰基。将完全活性的修饰酶施用于这种酶有缺陷并显示出许多Canavan病症状的小鼠。在这种动物模型中,脑酶活性水平有统计学上的显着提高,而模仿Canavan病患者的底物水平升高,底物水平却下降。这些结果表明,修饰的酶正进入大脑,并具有纠正这种代谢缺陷的功能。现在为长期研究设定了阶段,以优化这种酶替代方法以开发治疗方案。

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