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多蛋白胶原蛋白/角蛋白水凝胶促进了小鼠模型中受损骨骼肌的肌生成和血管生成。

Multiprotein collagen/keratin hydrogel promoted myogenesis and angiogenesis of injured skeletal muscles in a mouse model.

作者信息

Namjoo Atieh Rezaei, Hassani Ayla, Amini Hassan, Nazaryabrbekoh Fateme, Saghati Sepideh, Saadatlou Mohammad Ali Ebrahimi, Khoshfetrat Ali Baradar, Khosrowshahi Nafiseh Didar, Rahbarghazi Reza

机构信息

Stem Cell Research Center, Tabriz University of Medical Sciences, Imam Reza St, Golgasht St, Tabriz, Iran.

Chemical Engineering Faculty, Sahand University of Technology, Tabriz, 51335-1996, Iran.

出版信息

BMC Biotechnol. 2024 Apr 26;24(1):23. doi: 10.1186/s12896-024-00847-4.

Abstract

Volumetric loss is one of the challenging issues in muscle tissue structure that causes functio laesa. Tissue engineering of muscle tissue using suitable hydrogels is an alternative to restoring the physiological properties of the injured area. Here, myogenic properties of type I collagen (0.5%) and keratin (0.5%) were investigated in a mouse model of biceps femoris injury. Using FTIR, gelation time, and rheological analysis, the physicochemical properties of the collagen (Col)/Keratin scaffold were analyzed. Mouse C2C12 myoblast-laden Col/Keratin hydrogels were injected into the injury site and histological examination plus western blotting were performed to measure myogenic potential after 15 days. FTIR indicated an appropriate interaction between keratin and collagen. The blend of Col/Keratin delayed gelation time when compared to the collagen alone group. Rheological analysis revealed decreased stiffening in blended Col/Keratin hydrogel which is favorable for the extrudability of the hydrogel. Transplantation of C2C12 myoblast-laden Col/Keratin hydrogel to injured muscle tissues led to the formation of newly generated myofibers compared to cell-free hydrogel and collagen groups (p < 0.05). In the C2C12 myoblast-laden Col/Keratin group, a low number of CD31 cells with minimum inflammatory cells was evident. Western blotting indicated the promotion of MyoD in mice that received cell-laden Col/Keratin hydrogel compared to the other groups (p < 0.05). Despite the increase of the myosin cell-laden Col/Keratin hydrogel group, no significant differences were obtained related to other groups (p > 0.05). The blend of Col/Keratin loaded with myoblasts provides a suitable myogenic platform for the alleviation of injured muscle tissue.

摘要

体积损失是肌肉组织结构中具有挑战性的问题之一,会导致功能受损。使用合适的水凝胶进行肌肉组织工程是恢复受损区域生理特性的一种替代方法。在此,在股二头肌损伤的小鼠模型中研究了I型胶原蛋白(0.5%)和角蛋白(0.5%)的成肌特性。通过傅里叶变换红外光谱(FTIR)、凝胶化时间和流变学分析,分析了胶原蛋白(Col)/角蛋白支架的物理化学性质。将负载小鼠C2C12成肌细胞的Col/角蛋白水凝胶注射到损伤部位,并在15天后进行组织学检查和蛋白质免疫印迹分析以测量成肌潜力。FTIR表明角蛋白与胶原蛋白之间存在适当的相互作用。与单独的胶原蛋白组相比,Col/角蛋白混合物延长了凝胶化时间。流变学分析显示混合的Col/角蛋白水凝胶的硬化程度降低,这有利于水凝胶的可挤出性。与无细胞水凝胶和胶原蛋白组相比,将负载C2C12成肌细胞的Col/角蛋白水凝胶移植到受伤的肌肉组织中导致新生成的肌纤维形成(p < 0.05)。在负载C2C12成肌细胞的Col/角蛋白组中,可见少量CD31细胞且炎症细胞最少。蛋白质免疫印迹分析表明,与其他组相比,接受负载细胞的Col/角蛋白水凝胶的小鼠中MyoD得到促进(p < 0.05)。尽管负载肌球蛋白细胞的Col/角蛋白水凝胶组有所增加,但与其他组相比未获得显著差异(p > 0.05)。负载成肌细胞的Col/角蛋白混合物为减轻受损肌肉组织提供了合适的成肌平台。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/20eb/11055224/32923ecf42da/12896_2024_847_Fig1_HTML.jpg

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