Alexeev Vitali, Arita Machiko, Donahue Adele, Bonaldo Paolo, Chu Mon-Li, Igoucheva Olga
Stem Cell Res Ther. 2014 Feb 12;5(1):21. doi: 10.1186/scrt411.
Congenital muscular dystrophies (CMD) are a clinically and genetically heterogeneous group of neuromuscular disorders characterized by muscle weakness within the first two years of life. Collagen VI-related muscle disorders have recently emerged as one of the most common types of CMD. COL6 CMD is caused by deficiency and/or dysfunction of extracellular matrix (ECM) protein collagen VI. Currently, there is no specific treatment for this disabling and life-threatening disease. The primary cellular targets for collagen VI CMD therapy are fibroblasts in muscle, tendon and skin, as opposed to muscle cells for other types of muscular dystrophies. However, recent advances in stem cell research have raised the possibility that use of adult stem cells may provide dramatic new therapies for treatment of COL6 CMD.
Here, we developed a procedure for isolation of human stem cells from the adipose layer of neonatal skin. The adipose-derived stem cells (ADSC) were examined for expression of ECM and related genes using gene expression array analysis. The therapeutic potential of ADSC was assessed after a single intramuscular transplantation in collagen VI-deficient mice.
Analysis of primary cultures confirmed that established ADSC represent a morphologically homogenous population with phenotypic and functional features of adult mesenchymal stem cells. A comprehensive gene expression analysis showed that ADSC express a vast array of ECM genes. Importantly, it was observed that ADSC synthesize and secrete all three collagen VI chains, suggesting suitability of ADSC for COL6 CMD treatment. Furthermore, we have found that a single intramuscular transplantation of ADSC into Col6a1-/-Rag1-/- mice under physiological and cardiotoxin-induced injury/regeneration conditions results in efficient engraftment and migration of stem cells within the skeletal muscle. Importantly, we showed that ADSC can survive long-term and continuously secrete the therapeutic collagen VI protein missing in the mutant mice.
Overall, our findings suggest that stem cell therapy can potentially provide a new avenue for the treatment of COL6 CMD and other muscular disorders and injuries.
先天性肌营养不良(CMD)是一组临床和基因异质性的神经肌肉疾病,其特征是在生命的头两年内出现肌肉无力。与胶原蛋白VI相关的肌肉疾病最近已成为最常见的CMD类型之一。COL6 CMD是由细胞外基质(ECM)蛋白胶原蛋白VI的缺乏和/或功能障碍引起的。目前,对于这种致残且危及生命的疾病尚无特异性治疗方法。与其他类型的肌营养不良症以肌肉细胞为主要细胞靶点不同,胶原蛋白VI CMD治疗的主要细胞靶点是肌肉、肌腱和皮肤中的成纤维细胞。然而,干细胞研究的最新进展增加了使用成体干细胞可能为COL6 CMD治疗提供显著新疗法的可能性。
在此,我们开发了一种从新生儿皮肤脂肪层中分离人类干细胞的方法。使用基因表达阵列分析检测脂肪来源干细胞(ADSC)中ECM及相关基因的表达。在胶原蛋白VI缺陷小鼠单次肌肉内移植后评估ADSC的治疗潜力。
原代培养分析证实,已建立的ADSC代表具有成体间充质干细胞表型和功能特征的形态学均一群体。全面的基因表达分析表明,ADSC表达大量的ECM基因。重要的是,观察到ADSC合成并分泌所有三条胶原蛋白VI链,表明ADSC适用于COL6 CMD治疗。此外,我们发现,在生理和心脏毒素诱导的损伤/再生条件下,将ADSC单次肌肉内移植到Col6a1-/-Rag1-/-小鼠中,可导致干细胞在骨骼肌内有效植入和迁移。重要的是,我们表明ADSC可长期存活并持续分泌突变小鼠中缺失的治疗性胶原蛋白VI蛋白。
总体而言,我们的研究结果表明干细胞疗法可能为COL6 CMD及其他肌肉疾病和损伤的治疗提供新途径。
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