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Controlled local presentation of matrix proteins in microparticle-laden cell aggregates

机译:载有微粒的细胞聚集体中基质蛋白的受控局部表达

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摘要

Multi-cellular aggregates are found in healthy and diseased tissues, and while cell-cell contact is important for regulating many cell functions, cells also interact, to varying degrees, with extra-cellular matrix (ECM) proteins. Islets of Langerhans are one such example of cell aggregates in contact with ECM, both at the periphery of the cluster and dispersed throughout. While several studies have investigated the effect of reintroducing contact with ECM proteins on islet cell survival and function, the majority of these experiments only allow contact with the exterior cells. Thus, cell-culture platforms that enable the study of ECM-cell interactions throughout multi-cellular aggregates are of interest.Here, local presentation of ECM proteins was achieved using hydrogel microwell arrays to incorporate protein-laden microparticles during formation of MIN6 β-cell aggregates. Varying the microparticle seeding density reproducibly controlled the number of microparticles incorporated within three-dimensional aggregates (i.e., total amount of protein). Further, a relatively uniform spatial distribution of laminin- and fibronectin-coated microparticles was achieved throughout the x-, y-, and z-directions. Multiple ECM proteins were presented to β-cells in concert by incorporating two distinct populations of microparticles throughout the aggregates. Finally, scaling the microwell device dimensions allowed for the formation of two different sized cell-particle aggregates, ~80 and 160 μm in diameter. While the total number of microparticles incorporated per aggregate varied with size, the fraction of the aggregate occupied by microparticles was affected only by the microparticle seeding density, indicating that uniform local concentrations of proteins can be preserved while changing the overall aggregate dimensions.
机译:在健康和患病的组织中发现了多细胞聚集体,尽管细胞与细胞之间的接触对于调节许多细胞功能很重要,但细胞也会与细胞外基质(ECM)蛋白发生不同程度的相互作用。朗格汉斯岛就是这样一种例子,它既在簇的外围,又遍及整个细胞,与ECM接触。尽管有几项研究调查了重新引入与ECM蛋白接触对胰岛细胞存活和功能的影响,但这些实验中的大多数仅允许与外部细胞接触。因此,能够研究整个多细胞聚集体中ECM细胞相互作用的细胞培养平台引起了人们的兴趣。在这里,使用水凝胶微孔阵列在MIN6β细胞形成过程中掺入了载有蛋白质的微粒,实现了ECM蛋白的局部表达聚集体。改变微粒接种密度可再现地控制并入三维聚集体中的微粒数量(即蛋白质总量)。此外,在x,y和z方向上均获得了层粘连蛋白和纤连蛋白包被的微粒的相对均匀的空间分布。通过在整个聚集体中掺入两个不同的微粒群,多种ECM蛋白共同呈现给β细胞。最后,按比例缩放微孔装置尺寸允许形成两种不同大小的细胞颗粒聚集体,直径分别约为80和160μm。虽然每个聚集体掺入的微粒总数随尺寸而变化,但微粒所占聚集体的比例仅受微粒接种密度的影响,表明在改变总体聚集体尺寸的同时,可以保留蛋白质的均匀局部浓度。

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