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用于心血管应用的猪小肠黏膜下层细胞外基质的间充质干细胞接种

Mesenchymal Stem Cell Seeding of Porcine Small Intestinal Submucosal Extracellular Matrix for Cardiovascular Applications.

作者信息

Chang Chia Wei, Petrie Tye, Clark Alycia, Lin Xin, Sondergaard Claus S, Griffiths Leigh G

机构信息

Department of Medicine and Epidemiology, School of Veterinary Medicine, University of California, Davis, Davis, California, United States of America.

Department of Surgery, School of Medicine, University of California, Davis, Sacramento, California, United States of America.

出版信息

PLoS One. 2016 Apr 12;11(4):e0153412. doi: 10.1371/journal.pone.0153412. eCollection 2016.

Abstract

In this study, we investigate the translational potential of a novel combined construct using an FDA-approved decellularized porcine small intestinal submucosa extracellular matrix (SIS-ECM) seeded with human or porcine mesenchymal stem cells (MSCs) for cardiovascular indications. With the emerging success of individual component in various clinical applications, the combination of SIS-ECM with MSCs could provide additional therapeutic potential compared to individual components alone for cardiovascular repair. We tested the in vitro effects of MSC-seeding on SIS-ECM on resultant construct structure/function properties and MSC phenotypes. Additionally, we evaluated the ability of porcine MSCs to modulate recipient graft-specific response towards SIS-ECM in a porcine cardiac patch in vivo model. Specifically, we determined: 1) in vitro loading-capacity of human MSCs on SIS-ECM, 2) effect of cell seeding on SIS-ECM structure, compositions and mechanical properties, 3) effect of SIS-ECM seeding on human MSC phenotypes and differentiation potential, and 4) optimal orientation and dose of porcine MSCs seeded SIS-ECM for an in vivo cardiac application. In this study, histological structure, biochemical compositions and mechanical properties of the FDA-approved SIS-ECM biomaterial were retained following MSCs repopulation in vitro. Similarly, the cellular phenotypes and differentiation potential of MSCs were preserved following seeding on SIS-ECM. In a porcine in vivo patch study, the presence of porcine MSCs on SIS-ECM significantly reduced adaptive T cell response regardless of cell dose and orientation compared to SIS-ECM alone. These findings substantiate the clinical translational potential of combined SIS-ECM seeded with MSCs as a promising therapeutic candidate for cardiac applications.

摘要

在本研究中,我们调查了一种新型组合构建体的转化潜力,该构建体使用经美国食品药品监督管理局(FDA)批准的脱细胞猪小肠黏膜下层细胞外基质(SIS - ECM),接种人或猪间充质干细胞(MSC)用于心血管适应症。随着各个组件在各种临床应用中取得越来越多的成功,与单独使用单个组件相比,SIS - ECM与MSC的组合可能为心血管修复提供额外的治疗潜力。我们测试了在SIS - ECM上接种MSC对所得构建体结构/功能特性以及MSC表型的体外影响。此外,我们在猪心脏补片体内模型中评估了猪MSC调节受体对SIS - ECM的移植物特异性反应的能力。具体而言,我们确定了:1)人MSC在SIS - ECM上的体外负载能力,2)细胞接种对SIS - ECM结构、成分和力学性能的影响,3)SIS - ECM接种对人MSC表型和分化潜能的影响,以及4)用于体内心脏应用的接种猪MSC的SIS - ECM的最佳取向和剂量。在本研究中,经FDA批准的SIS - ECM生物材料在体外重新接种MSC后,其组织结构、生化成分和力学性能得以保留。同样,在接种到SIS - ECM上后,MSC的细胞表型和分化潜能也得以保留。在一项猪体内补片研究中,与单独的SIS - ECM相比,SIS - ECM上存在猪MSC显著降低了适应性T细胞反应,无论细胞剂量和取向如何。这些发现证实了接种MSC的组合SIS - ECM作为心脏应用中有前景的治疗候选物的临床转化潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/216e/4829265/4c3c6572583c/pone.0153412.g001.jpg

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