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异步性炎症和肌源性细胞迁移限制了由细胞支架介导的肌肉组织再生。

Asynchronous inflammation and myogenic cell migration limit muscle tissue regeneration mediated by a cellular scaffolds.

作者信息

Garg Koyal, Ward Catherine L, Corona Benjamin T

机构信息

United States Army Institute of Surgical Research, Extremity Trauma and Regenerative Medicine, USA; University of Illinois, Urbana Champaign, Beckman Institute of Advanced Science and Technology, USA.

United States Army Institute of Surgical Research, Extremity Trauma and Regenerative Medicine, USA.

出版信息

Inflamm Cell Signal. 2014;1(4). doi: 10.14800/ics.530. Epub 2015 Mar 10.

Abstract

Volumetric muscle loss (VML) following orthopaedic trauma results in chronic loss of strength and can contribute to disability. Tissue engineering and regenerative medicine approaches to regenerate the lost skeletal muscle and improve functional outcomes are currently under development. At the forefront of these efforts, decellularized extracellular matrices (ECMs) have reached clinical testing and provide the foundation for other approaches that include stem/progenitor cell delivery. ECMs have been demonstrated to possess many qualities to initiate regeneration, to include stem cell chemotaxis and pro-regenerative macrophage polarization. However, the majority of observations indicate that ECM-repair of VML does not promote appreciable muscle fiber regeneration. In a recent study, ECM-repair of VML was compared to muscle fiber regeneration (Garg ., 2014, Cell & Tissue Research) mediated by autologous minced grafts. The most salient findings of this study were: 1) Satellite cells did not migrate into the scaffold beyond ~0.5 mm from the remaining host tissue, although other migratory stem cells (Sca-1) were observed throughout the scaffold;2) Macrophage migration to the scaffold was over two-times that observed with muscle grafts, but they appeared to be less active, as gene expression of pro- and anti-inflammatory cytokines (TNF-α, IL-12, IL-4, IL-10, VEGF, and TGF-β1) was significantly reduced in scaffold-repaired muscles; And, 3) scaffolds did not promote appreciable muscle fiber regeneration. Collectively, these data suggest that the events following ECM transplantation in VML are either incongruous or asynchronous with muscle fiber regeneration.

摘要

骨科创伤后的容积性肌肉损失(VML)会导致长期的力量丧失,并可能导致残疾。目前正在开发组织工程和再生医学方法来再生受损的骨骼肌并改善功能结果。在这些努力的前沿,脱细胞细胞外基质(ECM)已进入临床试验,并为包括干细胞/祖细胞递送在内的其他方法提供了基础。ECM已被证明具有许多启动再生的特性,包括干细胞趋化性和促再生巨噬细胞极化。然而,大多数观察结果表明,ECM修复VML并不能促进明显的肌纤维再生。在最近的一项研究中,将VML的ECM修复与自体切碎移植物介导的肌纤维再生(Garg等人,2014年,《细胞与组织研究》)进行了比较。这项研究最显著的发现是:1)卫星细胞没有迁移到距剩余宿主组织约0.5毫米以外的支架中,尽管在整个支架中观察到了其他迁移干细胞(Sca-1);2)巨噬细胞向支架的迁移是肌肉移植的两倍多,但它们似乎不太活跃,因为支架修复肌肉中促炎和抗炎细胞因子(TNF-α、IL-12、IL-4、IL-10、VEGF和TGF-β1)的基因表达显著降低;3)支架没有促进明显的肌纤维再生。总体而言,这些数据表明,VML中ECM移植后的事件与肌纤维再生不一致或不同步。

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