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Recent advances in gene therapy for lysosomal storage disorders

机译:溶酶体贮积症基因治疗的最新进展

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摘要

Lysosomal storage disorders (LSDs) are a group of genetic diseases that result in metabolic derangements of the lysosome. Most LSDs are due to the genetic absence of a single catabolic enzyme, causing accumulation of the enzyme’s substrate within the lysosome. Over time, tissue-specific substrate accumulations result in a spectrum of symptoms and disabilities that vary by LSD. LSDs are promising targets for gene therapy because delivery of a single gene into a small percentage of the appropriate target cells may be sufficient to impact the clinical course of the disease. Recently, there have been several significant advancements in the potential for gene therapy of these disorders, including the first human trials. Future clinical trials will build upon these initial attempts, with an improved understanding of immune system responses to gene therapy, the obstacle that the blood–brain barrier poses for neuropathic LSDs, as well other biological barriers that, when overcome, may facilitate gene therapy for LSDs. In this manuscript, we will highlight the recent innovations in gene therapy for LSDs and discuss the clinical limitations that remain to be overcome, with the goal of fostering an understanding and further development of this important field.
机译:溶酶体贮积症(LSD)是一组遗传性疾病,可导致溶酶体的代谢紊乱。大多数LSD是由于单个分解代谢酶的基因缺失而引起的,导致酶的底物在溶酶体内积累。随着时间的流逝,组织特异性底物的积累会导致一系列症状和残疾,其随LSD的不同而变化。 LSD是基因治疗的有希望的靶标,因为将单个基因传递到一小部分适当的靶细胞中可能足以影响该疾病的临床进程。最近,包括首次人类试验在内,这些疾病的基因治疗潜力有了一些重大进展。未来的临床试验将以这些最初的尝试为基础,并加深对基因疗法的免疫系统反应的理解,血脑屏障对神经性LSD造成的障碍,以及克服时可能促进基因疗法的其他生物障碍。 LSD。在本手稿中,我们将重点介绍LSD基因治疗的最新创新,并讨论仍有待克服的临床局限性,以期加深对该重要领域的理解和进一步发展。

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