The giant striated muscle protein titin integrates into the developing sarcomere to form a stable myofilament system that is extended as myocytes fuse. The logistics underlying myofilament assembly and disassembly have started to emerge with the possibility to follow labeled sarcomere components. Here, we generated the mCherry knock-in at titin's Z-disk to study skeletal muscle development and remodeling. We find titin's integration into the sarcomere tightly regulated and its unexpected mobility facilitating a homogeneous distribution of titin after cell fusion - an integral part of syncytium formation and maturation of skeletal muscle. In adult mCherry-titin mice, treatment of muscle injury by implantation of titin-eGFP myoblasts reveals how myocytes integrate, fuse, and contribute to the continuous myofilament system across cell boundaries. Unlike in immature primary cells, titin proteins are retained at the proximal nucleus and do not diffuse across the whole syncytium with implications for future cell-based therapies of skeletal muscle disease.
Visualizing sarcomere and cellular dynamics in skeletal muscle to improve cell therapies.
通过可视化骨骼肌中的肌节和细胞动力学来改进细胞疗法
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作者:Hüttemeister Judith, Rudolph Franziska, Radke Michael H, Fink Claudia, Friedrich Dhana, Preibisch Stephan, Falcke Martin, Wagner Eva, Lehnart Stephan E, Gotthardt Michael
| 期刊: | Elife | 影响因子: | 6.400 |
| 时间: | 2024 | 起止号: | 2024 Dec 17; 13:e95597 |
| doi: | 10.7554/eLife.95597 | 研究方向: | 细胞生物学 |
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