人诱导多能干细胞衍生的间充质基质细胞在 Ullrich 先天性肌营养不良症模型小鼠中的独特肌肉再生能力。

Distinct muscle regenerative capacity of human induced pluripotent stem cell-derived mesenchymal stromal cells in Ullrich congenital muscular dystrophy model mice.

机构信息

Department of Clinical Application, Center for iPS Cell Research and Application, Kyoto University, 53 Kawahara-Cho, Shogoin, Sakyo-Ku, Kyoto, 606-8507, Japan.

Department of Rehabilitation Medicine, Nagoya City University Graduate School of Medical Sciences, 1 Kawasumi, Mizuho-Cho, Mizuho-Ku, Nagoya, 467-8601, Japan.

出版信息

Stem Cell Res Ther. 2024 Oct 7;15(1):340. doi: 10.1186/s13287-024-03951-6.

DOI:10.1186/s13287-024-03951-6

PMID:39370505

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11457425/

Abstract

BACKGROUND

Ullrich congenital muscular dystrophy (UCMD) is caused by a deficiency in type 6 collagen (COL6) due to mutations in COL6A1, COL6A2, or COL6A3. COL6 deficiency alters the extracellular matrix structure and biomechanical properties, leading to mitochondrial defects and impaired muscle regeneration. Therefore, mesenchymal stromal cells (MSCs) that secrete COL6 have attracted attention as potential therapeutic targets. Various tissue-derived MSCs exert therapeutic effects in various diseases. However, no reports have compared the effects of MSCs of different origins on UCMD pathology.

METHODS

To evaluate which MSC population has the highest therapeutic efficacy for UCMD, in vivo (transplantation of MSCs to Col6a1-KO/NSG mice) and in vitro experiments (muscle stem cell [MuSCs] co-culture with MSCs) were conducted using adipose tissue-derived MSCs, bone marrow-derived MSCs, and xeno-free-induced iPSC-derived MSCs (XF-iMSCs).

RESULTS

In transplantation experiments on Col6a1-KO/NSG mice, the group transplanted with XF-iMSCs showed significantly enhanced muscle fiber regeneration compared to the other groups 1 week after transplantation. At 12 weeks after transplantation, only the XF-iMSCs transplantation group showed a significantly larger muscle fiber diameter than the other groups without inducing fibrosis, which was observed in the other transplantation groups. Similarly, in co-culture experiments, XF-iMSCs were found to more effectively promote the fusion and differentiation of MuSCs derived from Col6a1-KO/NSG mice than the other primary MSCs investigated in this study. Additionally, in vitro knockdown and supplementation experiments suggested that the IGF2 secreted by XF-iMSCs promoted MuSC differentiation.

CONCLUSION

XF-iMSCs are promising candidates for promoting muscle regeneration while avoiding fibrosis, offering a safer and more effective therapeutic approach for UCMD than other potential therapies.

摘要

背景

先天性肌营养不良症（UCMD）是由于 COL6A1、COL6A2 或 COL6A3 基因突变导致 6 型胶原（COL6）缺乏引起的。COL6 缺乏会改变细胞外基质结构和生物力学特性，导致线粒体缺陷和肌肉再生受损。因此，分泌 COL6 的间充质基质细胞（MSCs）作为潜在的治疗靶点引起了关注。各种组织来源的 MSCs 在各种疾病中发挥治疗作用。然而，目前尚无研究比较不同来源的 MSCs 对 UCMD 病理的影响。

方法

为了评估哪种 MSC 群体对 UCMD 具有最高的治疗效果，我们进行了体内（将 MSCs 移植到 Col6a1-KO/NSG 小鼠）和体外实验（肌肉干细胞[MuSCs]与 MSCs 共培养），使用脂肪组织来源的 MSCs、骨髓来源的 MSCs 和无动物来源诱导的 iPSC 来源的 MSCs（XF-iMSCs）。

结果

在 Col6a1-KO/NSG 小鼠移植实验中，与其他组相比，移植 XF-iMSCs 的组在移植后 1 周时肌肉纤维再生明显增强。在移植后 12 周时，只有 XF-iMSCs 移植组的肌肉纤维直径明显大于其他组，而没有纤维化，而其他移植组则观察到纤维化。同样，在共培养实验中，与本研究中调查的其他原代 MSCs 相比，XF-iMSCs 更有效地促进了 Col6a1-KO/NSG 小鼠来源的 MuSCs 的融合和分化。此外，体外敲低和补充实验表明，XF-iMSCs 分泌的 IGF2 促进了 MuSC 的分化。