a Ultrastructural Pathology Laboratory , Victor Babes National Institute of Pathology , Bucharest , Romania.
b Department of Cellular & Molecular Biology and Histology , School of Medicine, Carol Davila University of Medicine and Pharmacy , Bucharest , Romania.
Cell Adh Migr. 2018 May 4;12(3):228-235. doi: 10.1080/19336918.2017.1346774. Epub 2017 Aug 30.
Regeneration in adult skeletal muscle relies on the activation, proliferation, and fusion of myogenic precursor cells (MPC), mostly resident satellite cells (SC). However, the regulatory mechanism during this process is still under evaluation, with the final aim to manipulate regeneration when the intrinsic mechanism is corrupted. Furthermore, intercellular connections during skeletal muscle regeneration have not been previously thoroughly documented. Our hypothesis was that a direct and close cellular interaction between SC/MPC and invading myeloid cells is a key step to control regeneration. We tested this hypothesis during different steps of skeletal muscle regeneration: (a) the recruitment of activated SC; (b) the differentiation of MPC; (c) myotubes growth, in a mouse model of crush injury. Samples harvested (3 and 5 days) post-injury were screened by light and confocal microscopy. Ultrastructural analysis was performed by conventional transmission electron microscopy (TEM) and scanning transmission electron microscopy (STEM) followed by 3D modeling of electron tomography (ET) data. This revealed a new type of interaction between macrophages and myogenic cells by direct heterocellular surface apposition over large areas and long linear distances. In the analyzed volume, regions spaced below 20 nm, within molecular range, represented 31% of the macrophage membrane surface and more than 27% of the myotube membrane. The constant interaction throughout all stages of myogenesis suggests a potential new type of regulatory mechanism for the myogenic process. Thus, deciphering structural and molecular mechanisms of SC-macrophage interaction following injury might open promising perspectives for improving muscle healing.
成体骨骼肌的再生依赖于肌源性前体细胞(MPC)的激活、增殖和融合,这些细胞主要是驻留的卫星细胞(SC)。然而,这个过程的调控机制仍在评估中,最终目的是在内在机制受损时操纵再生。此外,骨骼肌再生过程中的细胞间连接以前没有被详细记录。我们的假设是,SC/MPC 和浸润的髓系细胞之间的直接和密切的细胞相互作用是控制再生的关键步骤。我们在不同的骨骼肌再生阶段(a)激活的 SC 的募集;(b)MPC 的分化;(c)肌管生长,在小鼠挤压伤模型中测试了这个假设。损伤后 3 和 5 天采集的样本通过光镜和共聚焦显微镜进行筛选。超微结构分析通过常规透射电子显微镜(TEM)和扫描透射电子显微镜(STEM)进行,随后对电子断层扫描(ET)数据进行 3D 建模。这揭示了一种新的巨噬细胞和肌细胞之间的相互作用类型,通过直接的异细胞表面贴附和大的面积和长的线性距离。在分析的体积中,间隔小于 20nm 的区域,处于分子范围内,代表了巨噬细胞膜表面的 31%和肌管细胞膜表面的 27%以上。在整个肌发生阶段的持续相互作用表明,这种相互作用可能是肌发生过程的一种新的调节机制。因此,解析损伤后 SC-巨噬细胞相互作用的结构和分子机制可能为改善肌肉愈合开辟有前景的前景。
