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少即是多:溶酶体贮积症的底物减少疗法

Less Is More: Substrate Reduction Therapy for Lysosomal Storage Disorders.

作者信息

Coutinho Maria Francisca, Santos Juliana Inês, Alves Sandra

机构信息

Department of Human Genetics, Research and Development Unit, National Health Institute Doutor Ricardo Jorge, Rua Alexandre Herculano, 321 4000-055 Porto, Portugal.

出版信息

Int J Mol Sci. 2016 Jul 4;17(7):1065. doi: 10.3390/ijms17071065.

Abstract

Lysosomal storage diseases (LSDs) are a group of rare, life-threatening genetic disorders, usually caused by a dysfunction in one of the many enzymes responsible for intralysosomal digestion. Even though no cure is available for any LSD, a few treatment strategies do exist. Traditionally, efforts have been mainly targeting the functional loss of the enzyme, by injection of a recombinant formulation, in a process called enzyme replacement therapy (ERT), with no impact on neuropathology. This ineffectiveness, together with its high cost and lifelong dependence is amongst the main reasons why additional therapeutic approaches are being (and have to be) investigated: chaperone therapy; gene enhancement; gene therapy; and, alternatively, substrate reduction therapy (SRT), whose aim is to prevent storage not by correcting the original enzymatic defect but, instead, by decreasing the levels of biosynthesis of the accumulating substrate(s). Here we review the concept of substrate reduction, highlighting the major breakthroughs in the field and discussing the future of SRT, not only as a monotherapy but also, especially, as complementary approach for LSDs.

摘要

溶酶体贮积症(LSDs)是一组罕见的、危及生命的遗传性疾病,通常由负责溶酶体内消化的多种酶之一功能失调引起。尽管目前尚无治疗任何溶酶体贮积症的方法,但确实存在一些治疗策略。传统上,主要通过注射重组制剂来针对酶的功能丧失,这一过程称为酶替代疗法(ERT),但对神经病理学没有影响。这种无效性,连同其高成本和终身依赖性,是正在(且必须)研究其他治疗方法的主要原因之一:伴侣疗法;基因增强;基因治疗;另外还有底物减少疗法(SRT),其目的不是通过纠正原始酶缺陷来预防贮积,而是通过降低累积底物的生物合成水平来预防贮积。在此,我们回顾底物减少的概念,突出该领域的重大突破,并讨论底物减少疗法的未来,不仅作为单一疗法,特别是作为溶酶体贮积症的辅助疗法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/42b1/4964441/88503836861b/ijms-17-01065-g001.jpg

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