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Rehabilitative exercise and spatially patterned nanofibrillar scaffolds enhance vascularization and innervation following volumetric muscle loss.康复锻炼和空间图案化纳米纤维支架可增强容积性肌肉损失后的血管生成和神经支配。
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Decellularised skeletal muscles allow functional muscle regeneration by promoting host cell migration.去细胞化的骨骼肌通过促进宿主细胞迁移来实现功能性肌肉再生。
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Mesenchymal stem cells and extracellular matrix scaffold promote muscle regeneration by synergistically regulating macrophage polarization toward the M2 phenotype.间充质干细胞和细胞外基质支架通过协同调节巨噬细胞向 M2 表型极化来促进肌肉再生。
Stem Cell Res Ther. 2018 Apr 3;9(1):88. doi: 10.1186/s13287-018-0821-5.
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Co-delivery of a laminin-111 supplemented hyaluronic acid based hydrogel with minced muscle graft in the treatment of volumetric muscle loss injury.在治疗大面积肌肉损失损伤中,将补充了层粘连蛋白-111的透明质酸基水凝胶与肌肉碎块移植共同递送。
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An acellular biologic scaffold treatment for volumetric muscle loss: results of a 13-patient cohort study.一种用于治疗大面积肌肉损失的无细胞生物支架疗法:一项13例患者队列研究的结果。
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Co-delivery of micronized urinary bladder matrix damps regenerative capacity of minced muscle grafts in the treatment of volumetric muscle loss injuries.微细化尿囊素基质的共递送抑制了切碎肌肉移植物在容积性肌肉缺失损伤治疗中的再生能力。
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Bioengineered constructs combined with exercise enhance stem cell-mediated treatment of volumetric muscle loss.生物工程构建物与运动相结合可增强干细胞介导的容积性肌肉损失治疗效果。
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Age and sex differences in human skeletal muscle fibrosis markers and transforming growth factor-β signaling.人类骨骼肌纤维化标志物及转化生长因子-β信号传导中的年龄和性别差异。
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体积性肌肉损失损伤的再生修复对年龄敏感。

Regenerative Repair of Volumetric Muscle Loss Injury is Sensitive to Age.

机构信息

Department of Biomedical Engineering, University of Arkansas, Fayetteville, Arkansas.

Department of Health, Human Performance, and Recreation, College of Education and Health Professions, University of Arkansas, Fayetteville, Arkansas.

出版信息

Tissue Eng Part A. 2020 Jan;26(1-2):3-14. doi: 10.1089/ten.TEA.2019.0034. Epub 2019 Aug 9.

DOI:10.1089/ten.TEA.2019.0034
PMID:31064280
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6983754/
Abstract

In this study, the influence of age on effectiveness of regenerative repair for the treatment of volumetric muscle loss (VML) injury was explored. Tibialis anterior (TA) VML injuries were repaired in both 3- and 18-month-old animal models (Fischer 344 rat) using allogeneic decellularized skeletal muscle (DSM) scaffolds supplemented with autologous minced muscle (MM) paste. Within the 3-month animal group, TA peak contractile force was significantly improved (79% of normal) in response to DSM+MM repair. However, within the 18-month animal group, muscle force following repair (57% of normal) was not significantly different from unrepaired VML controls (59% of normal). Within the 3-month animal group, repair with DSM+MM generally reduced scarring at the site of VML repair, whereas scarring and a loss of contractile tissue was notable at the site of repair within the 18-month group. Within 3-month animals, expression of myogenic genes (, ), extracellular matrix genes (, , ), and key wound healing genes ( and ) were increased. Alternatively, expression was unchanged across all genes examined within the 18-month animal group. The findings suggest that a decline in regenerative capacity and increased fibrosis with age may present an obstacle to regenerative medicine strategies targeting VML injury. Impact Statement This study compared the recovery following volumetric muscle loss (VML) injury repair using a combination of minced muscle paste and decellularized muscle extracellular matrix carrier in both a younger (3 months) and older (18 months) rat population. Currently, VML repair research is being conducted with the young patient population in mind, but our group is the first to look at the effects of age on the efficacy of VML repair. Our findings highlight the importance of considering age-related changes in response to VML when developing repair strategies targeting an elderly patient population.

摘要

在这项研究中,探讨了年龄对再生修复治疗体积性肌肉损失(VML)损伤效果的影响。使用同种异体去细胞化骨骼肌(DSM)支架补充自体切碎肌肉(MM)糊剂,修复 3 个月和 18 个月大的动物模型(Fischer 344 大鼠)的胫骨前肌(TA)VML 损伤。在 3 个月龄动物组中,DSM+MM 修复后 TA 峰值收缩力显著提高(正常的 79%)。然而,在 18 个月龄动物组中,修复后的肌肉力量(正常的 57%)与未修复的 VML 对照组(正常的 59%)无显著差异。在 3 个月龄动物组中,DSM+MM 修复通常可减少 VML 修复部位的瘢痕形成,而在 18 个月龄动物组中,修复部位的瘢痕形成和收缩组织丢失则较为明显。在 3 个月龄动物中,肌生成基因(、)、细胞外基质基因(、、)和关键愈合基因(和)的表达增加。相反,在 18 个月龄动物组中,所有检测基因的表达均无变化。这些发现表明,随着年龄的增长,再生能力下降和纤维化增加可能成为针对 VML 损伤的再生医学策略的障碍。 研究意义 本研究比较了在年轻(3 个月)和老年(18 个月)大鼠群体中,使用切碎肌肉糊和去细胞化肌肉细胞外基质载体的组合修复体积性肌肉损失(VML)损伤后的恢复情况。目前,VML 修复研究主要针对年轻患者群体,但本研究小组是第一个研究年龄对 VML 修复效果的影响的小组。我们的研究结果强调了在制定针对老年患者群体的 VML 修复策略时,考虑到与年龄相关的 VML 反应的重要性。