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向预血管化胰岛微囊化装置迈出的重要一步:间质干细胞在微图案化膜上的体内预血管化。

An important step towards a prevascularized islet microencapsulation device: in vivo prevascularization by combination of mesenchymal stem cells on micropatterned membranes.

机构信息

Developmental BioEngineering, MIRA Institute of Biomedical Technology and Technical Medicine, University of Twente, Maastricht, The Netherlands.

(Bio)artificial organs. Department of Biomaterials Science and Technology, MIRA Institute of Biomedical Technology and Technical Medicine University of Twente, Maastricht, The Netherlands.

出版信息

J Mater Sci Mater Med. 2018 Nov 9;29(11):174. doi: 10.1007/s10856-018-6178-6.

Abstract

Extrahepatic transplantation of islets of Langerhans could aid in better survival of islets after transplantation. When islets are transfused into the liver 60-70% of them are lost immediately after transplantation. An important factor for a successful extrahepatic transplantation is a well-vascularized tissue surrounding the implant. There are many strategies known for enhancing vessel formation such as adding cells with endothelial potential, the combination with angiogenic factors and / or applying surface topography at the exposed surface of the device. Previously we developed porous, micropatterned membranes which can be applied as a lid for an islet encapsulation device and we showed that the surface topography induces human umbilical vein endothelial cell (HUVEC) alignment and interconnection. This was achieved without the addition of hydrogels, often used in angiogenesis assays. In this work, we went one step further towards clinical implementation of the device by combining this micropatterned lid with Mesenchymal Stem Cells (MSCs) to facilitate prevascularization in vivo. As for HUVECs, the micropatterned membranes induced MSC alignment and organization in vitro, an important contributor to vessel formation, whereas in vivo (subcutaneous rat model) they contributed to improved implant prevascularization. In fact, the combination of MSCs seeded on the micropatterned membrane induced the highest vessel formation score in 80% of the sections.

摘要

胰岛细胞的肝外移植可以帮助胰岛细胞在移植后更好地存活。当胰岛被输注到肝脏中时,其中 60-70%会在移植后立即丢失。肝外移植成功的一个重要因素是植入物周围有一个血管丰富的组织。有许多已知的策略可以促进血管形成,例如添加具有内皮潜能的细胞、与血管生成因子结合和/或在设备的暴露表面施加表面形貌。之前我们开发了多孔、微图案化的膜,可作为胰岛包封装置的盖子应用,我们表明表面形貌诱导人脐静脉内皮细胞(HUVEC)的排列和连接。这是在不添加水凝胶的情况下实现的,水凝胶通常用于血管生成测定中。在这项工作中,我们通过将这种微图案化的盖子与间充质干细胞(MSCs)结合,进一步将该设备推向临床实施,以促进体内的预血管生成。与 HUVEC 一样,微图案化膜在体外诱导 MSC 排列和组织,这是血管形成的一个重要贡献者,而在体内(皮下大鼠模型),它们有助于改善植入物的预血管生成。事实上,在微图案化膜上接种 MSCs 的组合在 80%的切片中诱导了最高的血管生成评分。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2f8a/6244873/14170f399eef/10856_2018_6178_Fig1_HTML.jpg

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