Engineered muscle from micro-channeled PEG scaffold with magnetic Fe3O4 fixation towards accelerating esophageal muscle repair

肌动蛋白 组织工程 再生(生物学) 心肌细胞 PEG比率 材料科学 肌球蛋白 纳米技术 脚手架 生物物理学 再生医学 细胞生物学 生物医学工程 干细胞 生物 医学 财务 经济
作者
Yang Luo,Yi‐Chen Chen,Zhaofeng Gu,Renhao Ni,Peipei Feng,Zeming Hu,Linlin Song,Xiang Shen,Chenjie Gu,Jiajie Li,Tianyu Du,Yang Lu,Hua Zhang,Yabin Zhu
出处
期刊:Materials today bio [Elsevier]
卷期号:23: 100853-100853
标识
DOI:10.1016/j.mtbio.2023.100853
摘要

Engineered scaffolds are used for repairing damaged esophagus to allow the precise alignment and movement of smooth muscle for peristalsis. However, most of these scaffolds focus solely on inducing cell alignment through directional apparatus, often overlooking the promotion of muscle tissue formation and causing reduced esophageal muscle repair effectiveness. To address this issue, we first introduced aligned nano-ferroferric oxide (Fe3O4) assemblies on a micropatterned poly(ethylene glycol) (PEG) hydrogel to form micro-/nano-stripes. Further modification using a gold coating was found to enhance cellular adhesion, orientation and organization within these micro-/nano-stripes, which consequently prevented excessive adhesion of smooth muscle cells (SMCs) to the thin PEG ridges, thereby effectively confining the cells to the Fe3O4-laid channels. This architectural design promotes the alignment of the cytoskeleton and elongation of actin filaments, leading to the organized formation of muscle bundles and a tendency for SMCs to adopt synthetic phenotypes. Muscle patches are harvested from the micro-/nano-stripes and transplanted into a rat esophageal defect model. In vivo experiments demonstrate the exceptional viability of these muscle patches and their ability to accelerate the regeneration of esophageal tissue. Overall, this study presents an efficient strategy for constructing muscle patches with directional alignment and muscle bundle formation of SMCs, holding significant promise for muscle tissue regeneration.
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