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聚唾液酸在中枢神经系统修复中的应用。

Use of polysialic acid in repair of the central nervous system.

作者信息

El Maarouf Abderrahman, Petridis Athanasios K, Rutishauser Urs

机构信息

Laboratory of Cellular and Developmental Neuroscience, Department of Cell Biology, Memorial Sloan-Kettering Cancer Center, 1275 York Avenue, New York, NY 10021, USA.

出版信息

Proc Natl Acad Sci U S A. 2006 Nov 7;103(45):16989-94. doi: 10.1073/pnas.0608036103. Epub 2006 Oct 30.

Abstract

Polysialic acid (PSA), a large cell-surface carbohydrate that regulates cell interactions, is used during vertebrate development to promote precursor cell migration and axon path-finding. The induction of PSA expression in damaged adult CNS tissues could help them to rebuild by creating conditions permissive for architectural remodeling. This possibility has been explored in two contexts, the regeneration of axons and the recruitment of endogenous neural precursors to a lesion. Glial scars that form at CNS injury sites block axon regeneration. It has been found that transfection of scar astrocytes by a viral vector encoding polysialyltransferase leads to sustained expression of high levels of PSA. With this treatment, a substantial portion of severed corticospinal tract axon processes were able to grow through a spinal injury site. In the studies of precursor cell migration to a cortical lesion, it was found that induced PSA expression in a path extending from the subventricular zone to a lesion near the cortical surface increased recruitment of BrdU/nestin-positive cells along the path and into the injury site. These displaced precursors were able to differentiate in a regionally appropriate manner. These findings suggest that induced PSA expression can be used as a strategy for promoting tissue repair involving both replacement of cells and rebuilding of neural connections.

摘要

多唾液酸(PSA)是一种调节细胞间相互作用的大型细胞表面碳水化合物,在脊椎动物发育过程中用于促进前体细胞迁移和轴突寻路。在受损的成体中枢神经系统组织中诱导PSA表达,可通过创造有利于结构重塑的条件来帮助它们重建。这种可能性已在两种情况下进行了探索,即轴突再生和内源性神经前体细胞向损伤部位的募集。中枢神经系统损伤部位形成的胶质瘢痕会阻碍轴突再生。已发现用编码多唾液酸转移酶的病毒载体转染瘢痕星形胶质细胞可导致高水平PSA的持续表达。通过这种治疗,相当一部分切断的皮质脊髓束轴突能够穿过脊髓损伤部位生长。在对前体细胞向皮质损伤部位迁移的研究中,发现从脑室下区延伸至皮质表面附近损伤部位的路径中诱导PSA表达,可增加沿该路径并进入损伤部位的BrdU/巢蛋白阳性细胞的募集。这些迁移来的前体细胞能够以区域合适的方式分化。这些发现表明,诱导PSA表达可作为一种促进组织修复的策略,涉及细胞替代和神经连接重建。

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