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基于神经胶质前体细胞的儿童脑白质营养不良治疗方法

Glial progenitor cell-based treatment of the childhood leukodystrophies.

作者信息

Osorio M Joana, Goldman Steven A

机构信息

Center for Translational Neuromedicine, University of Rochester Medical Center, Rochester, NY 14642, United States; Center for Basic and Translational Neuroscience, University of Copenhagen Faculty of Health and Medical Sciences, Copenhagen 2200, Denmark.

出版信息

Exp Neurol. 2016 Sep;283(Pt B):476-88. doi: 10.1016/j.expneurol.2016.05.010. Epub 2016 May 8.

Abstract

The childhood leukodystrophies comprise a group of hereditary disorders characterized by the absence, malformation or destruction of myelin. These disorders share common clinical, radiological and pathological features, despite their diverse molecular and genetic etiologies. Oligodendrocytes and astrocytes are the major affected cell populations, and are either structurally impaired or metabolically compromised through cell-intrinsic pathology, or are the victims of mis-accumulated toxic byproducts of metabolic derangement. In either case, glial cell replacement using implanted tissue or pluripotent stem cell-derived human neural or glial progenitor cells may comprise a promising strategy for both structural remyelination and metabolic rescue. A broad variety of pediatric white matter disorders, including the primary hypomyelinating disorders, the lysosomal storage disorders, and the broader group of non-lysosomal metabolic leukodystrophies, may all be appropriate candidates for glial progenitor cell-based treatment. Nonetheless, a variety of specific challenges remain before this therapeutic strategy can be applied to children. These include timely diagnosis, before irreparable neuronal injury has ensued; understanding the natural history of the targeted disease; defining the optimal cell phenotype for each disorder; achieving safe and scalable cellular compositions; designing age-appropriate controlled clinical trials; and for autologous therapy of genetic disorders, achieving the safe genetic editing of pluripotent stem cells. Yet these challenges notwithstanding, the promise of glial progenitor cell-based treatment of the childhood myelin disorders offers hope to the many victims of this otherwise largely untreatable class of disease.

摘要

儿童脑白质营养不良是一组遗传性疾病,其特征为髓鞘缺失、畸形或破坏。尽管这些疾病的分子和遗传病因各不相同,但它们具有共同的临床、放射学和病理学特征。少突胶质细胞和星形胶质细胞是主要受影响的细胞群体,它们要么因细胞内在病理而在结构上受损或代谢受到影响,要么是代谢紊乱产生的有毒副产物错误积累的受害者。在任何一种情况下,使用植入组织或多能干细胞衍生的人类神经或神经胶质祖细胞进行胶质细胞替代,可能是结构再髓鞘化和代谢挽救的一种有前景的策略。多种儿科白质疾病,包括原发性髓鞘形成障碍、溶酶体贮积病以及更广泛的非溶酶体代谢性脑白质营养不良,都可能是基于胶质祖细胞治疗的合适候选者。然而,在将这种治疗策略应用于儿童之前,仍存在各种具体挑战。这些挑战包括在不可修复的神经元损伤发生之前及时诊断;了解目标疾病的自然史;确定每种疾病的最佳细胞表型;实现安全且可扩展的细胞组成;设计适合年龄的对照临床试验;对于遗传性疾病的自体治疗,实现多能干细胞的安全基因编辑。尽管存在这些挑战,但基于胶质祖细胞治疗儿童髓鞘疾病的前景为这类原本大多无法治疗的疾病的众多受害者带来了希望。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/05d2/5340082/3bf94a67b3c2/nihms844818f1.jpg

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