Rhoads R P, Johnson R M, Rathbone C R, Liu X, Temm-Grove C, Sheehan S M, Hoying J B, Allen R E
Muscle Biology Group, Department of Animal Sciences, University of Arizona, Tucson, AZ 85721, USA.
Am J Physiol Cell Physiol. 2009 Jun;296(6):C1321-8. doi: 10.1152/ajpcell.00391.2008. Epub 2009 Apr 22.
Muscle regeneration involves the coordination of myogenesis and revascularization to restore proper muscle function. Myogenesis is driven by resident stem cells termed satellite cells (SC), whereas angiogenesis arises from endothelial cells and perivascular cells of preexisting vascular segments and the collateral vasculature. Communication between myogenic and angiogenic cells seems plausible, especially given the number of growth factors produced by SC. To characterize these interactions, we developed an in vitro coculture model composed of rat skeletal muscle SC and microvascular fragments (MVF). In this system, isolated epididymal MVF suspended in collagen gel are cultured over a rat SC monolayer culture. In the presence of SC, MVF exhibit greater indices of angiogenesis than MVF cultured alone. A positive dose-dependent effect of SC conditioned medium (CM) on MVF growth was observed, suggesting that SC secrete soluble-acting growth factor(s). Next, we specifically blocked VEGF action in SC CM, and this was sufficient to abolish satellite cell-induced angiogenesis. Finally, hypoxia-inducible factor-1alpha (HIF-1alpha), a transcriptional regulator of VEGF gene expression, was found to be expressed in cultured SC and in putative SC in sections of in vivo stretch-injured rat muscle. Hypoxic culture conditions increased SC HIF-1alpha activity, which was positively associated with SC VEGF gene expression and protein levels. Collectively, these initial observations suggest that a heretofore unexplored aspect of satellite cell physiology is the initiation of a proangiogenic program.
肌肉再生涉及肌生成和血管再生的协调,以恢复正常的肌肉功能。肌生成由称为卫星细胞(SC)的驻留干细胞驱动,而血管生成则源于现有血管段和侧支血管的内皮细胞及血管周围细胞。肌生成细胞与血管生成细胞之间的通讯似乎是合理的,特别是考虑到卫星细胞产生的生长因子数量。为了表征这些相互作用,我们开发了一种由大鼠骨骼肌卫星细胞和微血管片段(MVF)组成的体外共培养模型。在这个系统中,悬浮在胶原凝胶中的分离附睾微血管片段在大鼠卫星细胞单层培养物上进行培养。在卫星细胞存在的情况下,微血管片段比单独培养的微血管片段表现出更高的血管生成指标。观察到卫星细胞条件培养基(CM)对微血管片段生长具有剂量依赖性的积极作用,这表明卫星细胞分泌可溶性生长因子。接下来,我们特异性阻断了卫星细胞条件培养基中的VEGF作用,这足以消除卫星细胞诱导的血管生成。最后,发现缺氧诱导因子-1α(HIF-1α),一种VEGF基因表达的转录调节因子,在培养的卫星细胞以及体内拉伸损伤大鼠肌肉切片中的假定卫星细胞中表达。缺氧培养条件增加了卫星细胞HIF-1α活性,这与卫星细胞VEGF基因表达和蛋白水平呈正相关。总的来说,这些初步观察结果表明,卫星细胞生理学中一个迄今未被探索的方面是启动促血管生成程序。