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利用脂肪干细胞生成龛位调谐抗纤维化成纤维细胞和非病毒介导的内皮细胞定向分化,用于皮肤移植物的开发。

Generation of niche tuned antifibrotic fibroblasts and non-viral mediated endothelial commitment using adipose stem cells for dermal graft development.

机构信息

Division of Thrombosis Research, Department of Applied Biology, Biomedical Technology Wing, Sree Chitra Tirunal Institute for Medical Sciences and Technology (SCTIMST), Thiruvananthapuram, India.

Integrated Cancer Research, Rajiv Gandhi Centre for Biotechnology (RGCB), Thiruvananthapuram, India.

出版信息

J Biomed Mater Res B Appl Biomater. 2020 Oct;108(7):2807-2819. doi: 10.1002/jbm.b.34611. Epub 2020 Apr 3.

Abstract

Cell-based skin substitute generation has seen considerable development. Combining synthetic scaffolds with biomimetic fibrin does direct both exogenous and endogenous stem cell differentiation, addressing needs for reliable tissue engineering. However, lack of immediate vasculature within implantable grafts remains critical for its sustenance and integration. Multipotency, high proliferation potential, ability to release multiple growth factors (GFs), and autologous availability highlight the use of human adipose derived mesenchymal stem cells (hADMSCs) in tissue-engineered dermal grafts (TEDG) construction. However, hADMSCs' insufficiency to independently establish angiogenesis within tissue constructs demands improvement of stem cell application for dermal graft survival. Approaches to harness microenvironmentally sensitive paracrine interactions could improve the angiogenic efficiency of hADMSCs within TEDG. This study conceptualized a fibrin-based niche, to direct hADMSCs toward a nonfibrotic fibroblast commitment and incorporation of bioengineered hADMSCs, specifically releasing potent angiogenic factors within TEDG. Coexistence of tuned fibroblast and endothelial lineage committed cells contributed to well-regulated extracellular matrix formation and prevascularization. Adequate cell proliferation; sustained transient release of angiogenic GFs till 20 days; directed dermal, endothelial, fibroblast, and vascular smooth muscle cell differentiation; and favored elastin and collagen deposition were achieved in vitro. In conclusion, specific niche composition and employment of bioengineered hADMSCs favor implantable TEDG construction.

摘要

基于细胞的皮肤替代物的生成已经取得了相当大的发展。将合成支架与仿生纤维蛋白结合使用,可以直接引导外源性和内源性干细胞分化,满足可靠的组织工程需求。然而,可植入移植物内缺乏即时血管仍然是其维持和整合的关键。多功能性、高增殖潜力、能够释放多种生长因子 (GFs) 以及自体可用性突出了人脂肪来源间充质干细胞 (hADMSCs) 在组织工程真皮移植物 (TEDG) 构建中的应用。然而,hADMSCs 不足以独立在组织构建物中建立血管生成,这就需要改进干细胞在真皮移植物存活中的应用。利用微环境敏感的旁分泌相互作用的方法可以提高 TEDG 中 hADMSCs 的血管生成效率。本研究构建了一种基于纤维蛋白的小生境,以指导 hADMSCs 向非纤维性成纤维细胞方向分化,并将生物工程 hADMSCs 整合到 TEDG 中,特别是在 TEDG 中释放有效的血管生成因子。调谐的成纤维细胞和内皮谱系定向细胞的共存有助于调控良好的细胞外基质形成和血管前形成。体外实验中实现了足够的细胞增殖、持续释放短暂的血管生成 GF 长达 20 天、定向真皮、内皮、成纤维细胞和血管平滑肌细胞分化以及有利于弹性蛋白和胶原蛋白沉积。总之,特定小生境的组成和生物工程 hADMSCs 的应用有利于可植入 TEDG 的构建。

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