Muscle progenitor cells are required for skeletal muscle regeneration and prevention of adipogenesis after limb ischemia

肌肉祖细胞是骨骼肌再生和预防肢体缺血后脂肪生成所必需的

阅读:8
作者:Hasan Abbas, Lindsey A Olivere, Michael E Padgett, Cameron A Schmidt, Brian F Gilmore, Timothy J McCord, Kevin W Southerland, Joseph M McClung, Christopher D Kontos
期刊:Frontiers in Cardiovascular Medicine影响因子:2.800
时间:2023起止号:2023 Mar 2:10:1118738.
doi:10.3389/fcvm.2023.1118738种属: Goat
方法学: ELISA靶点: IgG Fc
研究方向: 细胞生物学细胞类型: 其它细胞

Abstract

Skeletal muscle injury in peripheral artery disease (PAD) has been attributed to vascular insufficiency, however evidence has demonstrated that muscle cell responses play a role in determining outcomes in limb ischemia. Here, we demonstrate that genetic ablation of Pax7+ muscle progenitor cells (MPCs) in a model of hindlimb ischemia (HLI) inhibited muscle regeneration following ischemic injury, despite a lack of morphological or physiological changes in resting muscle. Compared to control mice (Pax7WT), the ischemic limb of Pax7-deficient mice (Pax7Δ) was unable to generate significant force 7 or 28 days after HLI. A significant increase in adipose was observed in the ischemic limb 28 days after HLI in Pax7Δ mice, which replaced functional muscle. Adipogenesis in Pax7Δ mice corresponded with a significant increase in PDGFRα+ fibro/adipogenic progenitors (FAPs). Inhibition of FAPs with batimastat decreased muscle adipose but increased fibrosis. In vitro, Pax7Δ MPCs failed to form myotubes but displayed increased adipogenesis. Skeletal muscle from patients with critical limb threatening ischemia displayed increased adipose in more ischemic regions of muscle, which corresponded with fewer satellite cells. Collectively, these data demonstrate that Pax7+ MPCs are required for muscle regeneration after ischemia and suggest that muscle regeneration may be an important therapeutic target in PAD.

特别声明

1、本页面内容包含部分的内容是基于公开信息的合理引用;引用内容仅为补充信息,不代表本站立场。

2、若认为本页面引用内容涉及侵权,请及时与本站联系,我们将第一时间处理。

3、其他媒体/个人如需使用本页面原创内容,需注明“来源:[生知库]”并获得授权;使用引用内容的,需自行联系原作者获得许可。

4、投稿及合作请联系:info@biocloudy.com。