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双过氧钒,一种磷酸酪氨酸磷酸酶抑制剂,可使成肌细胞重编程以获得多能的循环表型。

Bisperoxovanadium, a phospho-tyrosine phosphatase inhibitor, reprograms myogenic cells to acquire a pluripotent, circulating phenotype.

作者信息

Castaldi L, Serra C, Moretti F, Messina G, Paoletti R, Sampaolesi M, Torgovnick A, Baiocchi M, Padula F, Pisaniello A, Molinaro M, Cossu G, Levrero M, Bouché M

机构信息

Department of Histology and Med. Embr., Univ. of Rome La Sapienza, Via A. Scarpa 14, 00161 Rome, Italy.

出版信息

FASEB J. 2007 Nov;21(13):3573-83. doi: 10.1096/fj.06-7454com. Epub 2007 Jun 29.

DOI:10.1096/fj.06-7454com
PMID:17601985
Abstract

Satellite cells are the main source of myogenic progenitors in postnatal skeletal muscle, but their use in cell therapy for muscle disorders is limited because these cells cannot be delivered through circulation and they are rapidly exhausted in severe myopathies. The search for alternative donor cells is ongoing, but none of the candidates so far show all the features required for successful colonization and repair of diseased muscle. In this study, we show that bisperoxovanadium, a phospho-tyrosine phosphatase inhibitor, induces myogenic cells to acquire a gene expression profile and a differentiation potential consistent with the phenotype of a circulating precursors, while maintaining their myogenic potential. These effects are mediated, at least in part, by NF-kappaB activation through the Tyr42-IkappaB-alpha phosphorylation, as shown by the expression of the dominant negative mutant form of the p50 NF-kappaB subunit. Moreover, when bisperoxovanadium-treated cells are injected into the femoral artery of alpha-sarcoglican null dystrophic mice, they are able to circulate and to reach muscle tissue; importantly, they contribute to muscle regeneration, as shown by the expression of alpha-sarcoglican in some fibers. Our observations indicate that bisperoxovanadium, or similar compounds, may prove very valuable to obtain and to expand, from committed cells, multipotent cell populations suitable for gene-cell therapy applications and may help to understand the molecular basis of genome reprogramming and "stem-ness."

摘要

卫星细胞是出生后骨骼肌中肌源性祖细胞的主要来源,但它们在用于肌肉疾病的细胞治疗时受到限制,因为这些细胞无法通过血液循环输送,并且在严重的肌病中会迅速耗尽。寻找替代供体细胞的工作正在进行,但到目前为止,没有一种候选细胞具备成功定殖和修复患病肌肉所需的所有特征。在本研究中,我们发现双过氧钒(一种磷酸酪氨酸磷酸酶抑制剂)可诱导肌源性细胞获得与循环前体细胞表型一致的基因表达谱和分化潜能,同时保持其肌源性潜能。这些效应至少部分是由通过Tyr42-IκB-α磷酸化激活NF-κB介导的,如p50 NF-κB亚基的显性负突变体形式的表达所示。此外,当将经双过氧钒处理的细胞注射到α-肌聚糖缺失的营养不良小鼠的股动脉中时,它们能够循环并到达肌肉组织;重要的是,如一些纤维中α-肌聚糖的表达所示,它们有助于肌肉再生。我们观察结果表明,双过氧钒或类似化合物可能对于从定向细胞中获得并扩增适用于基因-细胞治疗应用的多能细胞群体非常有价值,并且可能有助于理解基因组重编程和“干性”的分子基础。

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