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经设计可支持间充质干细胞 (MSC) 存活和增殖的微胶囊可使 MSCs 在梗死心肌中长期保留。

Microcapsules engineered to support mesenchymal stem cell (MSC) survival and proliferation enable long-term retention of MSCs in infarcted myocardium.

机构信息

Singapore Bioimaging Consortium (SBIC), Biomedical Sciences Institute, Agency for Science, Technology and Research (A*STAR), Singapore.

Singapore MIT Alliance for Research and Technology (SMART), BioSyM Interdisciplinary Research Group, Singapore.

出版信息

Biomaterials. 2015 Jun;53:12-24. doi: 10.1016/j.biomaterials.2015.02.075. Epub 2015 Mar 7.

DOI:10.1016/j.biomaterials.2015.02.075
PMID:25890702
Abstract

The limited efficacy of cardiac cell-based therapy is thought to be due to poor cell retention within the myocardium. Hence, there is an urgent need for biomaterials that aid in long-term cell retention. This study describes the development of injectable microcapsules for the delivery of mesenchymal stem cells (MSCs) into the infarcted cardiac wall. These microcapsules comprise of low concentrations of agarose supplemented with extracellular matrix (ECM) proteins collagen and fibrin. Dextran sulfate, a negatively charged polycarbohydrate, was added to mimic glycosaminoglycans in the ECM. Cell viability assays showed that a combination of all components is necessary to support long-term survival and proliferation of MSCs within microcapsules. Following intramyocardial transplantation, microcapsules degraded slowly in vivo and did not induce a fibrotic foreign body response. Pre-labeling of encapsulated MSCs with iron oxide nanoparticles allowed continued cell-tracking by MRI over several weeks following transplantation into infarcted myocardium. In contrast, MSCs injected as cell suspension were only detectable for two days post transplantation by MRI. Histological analysis confirmed integration of transplanted cells at the infarct site. Therefore, microcapsules proved to be suitable for stem cell delivery into the infarcted myocardium and can overcome current limitations of poor cell retention in cardiac cell-based therapy.

摘要

基于心脏细胞的治疗效果有限,被认为是由于细胞在心肌内的保留率差。因此,迫切需要能够帮助长期保留细胞的生物材料。本研究描述了用于将间充质干细胞(MSCs)递送至梗塞的心脏壁内的可注射微胶囊的开发。这些微胶囊包含低浓度的琼脂糖,辅以细胞外基质(ECM)蛋白胶原和纤维蛋白。葡聚糖硫酸盐,一种带负电荷的多糖,被添加以模拟 ECM 中的糖胺聚糖。细胞活力测定表明,所有成分的组合对于支持微胶囊内 MSC 的长期存活和增殖是必要的。在心肌内移植后,微胶囊在体内缓慢降解,并且不会引起纤维状异物反应。预先用氧化铁纳米颗粒标记包封的 MSC,允许在移植到梗塞的心肌后通过 MRI 进行数周的连续细胞追踪。相比之下,作为细胞悬浮液注射的 MSC 通过 MRI 在移植后仅可检测到两天。组织学分析证实了移植细胞在梗塞部位的整合。因此,微胶囊被证明适合将干细胞递送至梗塞的心肌内,并且可以克服心脏细胞治疗中目前存在的细胞保留率差的限制。

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