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肌肉干细胞的分离、鉴定和分子调控。

Isolation, characterization, and molecular regulation of muscle stem cells.

机构信息

Laboratory of Molecular and Cellular Physiology, Graduate School of Pharmaceutical Sciences, Osaka University Osaka, Japan.

出版信息

Front Physiol. 2013 Nov 12;4:317. doi: 10.3389/fphys.2013.00317. eCollection 2013.

Abstract

Skeletal muscle has great regenerative capacity which is dependent on muscle stem cells, also known as satellite cells. A loss of satellite cells and/or their function impairs skeletal muscle regeneration and leads to a loss of skeletal muscle power; therefore, the molecular mechanisms for maintaining satellite cells in a quiescent and undifferentiated state are of great interest in skeletal muscle biology. Many studies have demonstrated proteins expressed by satellite cells, including Pax7, M-cadherin, Cxcr4, syndecan3/4, and c-met. To further characterize satellite cells, we established a method to directly isolate satellite cells using a monoclonal antibody, SM/C-2.6. Using SM/C-2.6 and microarrays, we measured the genes expressed in quiescent satellite cells and demonstrated that Hesr3 may complement Hesr1 in generating quiescent satellite cells. Although Hesr1- or Hesr3-single knockout mice show a normal skeletal muscle phenotype, including satellite cells, Hesr1/Hesr3-double knockout mice show a gradual decrease in the number of satellite cells and increase in regenerative defects dependent on satellite cell numbers. We also observed that a mouse's genetic background affects the regenerative capacity of its skeletal muscle and have established a line of DBA/2-background mdx mice that has a much more severe phenotype than the frequently used C57BL/10-mdx mice. The phenotype of DBA/2-mdx mice also seems to depend on the function of satellite cells. In this review, we summarize the methodology of direct isolation, characterization, and molecular regulation of satellite cells based on our results. The relationship between the regenerative capacity of satellite cells and progression of muscular disorders is also summarized. In the last part, we discuss application of the accumulating scientific information on satellite cells to treatment of patients with muscular disorders.

摘要

骨骼肌具有很强的再生能力,这依赖于肌肉干细胞,也称为卫星细胞。卫星细胞的丧失和/或其功能障碍会损害骨骼肌的再生,导致骨骼肌力量的丧失;因此,维持卫星细胞处于静止和未分化状态的分子机制是骨骼肌生物学中的一个重要研究方向。许多研究已经证明了卫星细胞表达的蛋白质,包括 Pax7、M-cadherin、Cxcr4、 syndecan3/4 和 c-met。为了进一步表征卫星细胞,我们建立了一种使用单克隆抗体 SM/C-2.6 直接分离卫星细胞的方法。使用 SM/C-2.6 和微阵列,我们测量了静止卫星细胞中表达的基因,并证明 Hesr3 可能与 Hesr1 一起产生静止卫星细胞。尽管 Hesr1 或 Hesr3 单敲除小鼠表现出正常的骨骼肌表型,包括卫星细胞,但 Hesr1/Hesr3 双敲除小鼠表现出卫星细胞数量逐渐减少,再生缺陷增加,这取决于卫星细胞的数量。我们还观察到,老鼠的遗传背景会影响其骨骼肌的再生能力,我们已经建立了一条 DBA/2 背景的 mdx 小鼠系,其表型比常用的 C57BL/10-mdx 小鼠严重得多。DBA/2-mdx 小鼠的表型似乎也依赖于卫星细胞的功能。在这篇综述中,我们根据我们的结果总结了直接分离、表征和分子调控卫星细胞的方法。我们还总结了卫星细胞的再生能力与肌肉疾病进展之间的关系。在最后一部分,我们讨论了将关于卫星细胞的不断积累的科学信息应用于治疗肌肉疾病患者的问题。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d505/3824104/b961bce2ff5c/fphys-04-00317-g0001.jpg

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