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首页> 外文期刊>Biomaterials >An acellular biologic scaffold does not regenerate appreciable de novo muscle tissue in rat models of volumetric muscle loss injury
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An acellular biologic scaffold does not regenerate appreciable de novo muscle tissue in rat models of volumetric muscle loss injury

机译:脱细胞生物支架不能在大鼠容量性肌肉丢失损伤模型中再生明显的新生肌肉组织

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摘要

Extracellular matrix (ECM) derived scaffolds continue to be investigated for the treatment of volumetric muscle loss (VML) injuries. Clinically, ECM scaffolds have been used for lower extremity VML repair; in particular, MatriStem (TM), a porcine urinary bladder matrix (UBM), has shown improved functional outcomes and vascularization, but limited myogenesis. However, efficacy of the scaffold for the repair of traumatic muscle injuries has not been examined systematically. In this study, we demonstrate that the porcine UBM scaffold when used to repair a rodent gastrocnemius musculotendinous junction (MTJ) and tibialis anterior (TA) VML injury does not support muscle tissue regeneration. In the MTJ model, the scaffold was completely resorbed without tissue remodeling, suggesting that the scaffold may not be suitable for the clinical repair of muscle-tendon injuries. In the TA VML injury, the scaffold remodeled into a fibrotic tissue and showed functional improvement, but not due to muscle fiber regeneration. The inclusion of physical rehabilitation also did not improve functional response or tissue remodeling. We conclude that the porcine UBM scaffold when used to treat VML injuries may hasten the functional recovery through the mechanism of scaffold mediated functional fibrosis. Thus for appreciable muscle regeneration, repair strategies that incorporate myogenic cells, vasculogenic accelerant and a myoconductive scaffold need to be developed. Published by Elsevier Ltd.
机译:继续研究细胞外基质(ECM)衍生的支架治疗体积性肌肉丢失(VML)损伤的方法。临床上,ECM支架已用于下肢VML修复。尤其是,猪膀胱基质(UBM)的MatriStem(TM)已显示出改善的功能结局和血管生成,但肌生成受限。然而,尚未系统检查支架在修复外伤性肌肉损伤中的功效。在这项研究中,我们证明了猪UBM支架在修复啮齿类腓肠肌肌腱连接点(MTJ)和胫骨前(TA)VML损伤时不支持肌肉组织再生。在MTJ模型中,支架被完全吸收而没有组织重塑,表明该支架可能不适合肌腱损伤的临床修复。在TA VML损伤中,支架重塑为纤维化组织并显示功能改善,但不是由于肌纤维再生。包括身体康复也不能改善功能反应或组织重塑。我们得出的结论是,猪UBM支架在治疗VML损伤时可通过支架介导的功能性纤维化机制加快功能恢复。因此,对于明显的肌肉再生,需要开发结合肌细胞,血管生成促进剂和肌导支架的修复策略。由Elsevier Ltd.发布

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