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用于分析仿生细胞外基质特性的地形和肽功能化水凝胶阵列。

Arrays of topographically and peptide-functionalized hydrogels for analysis of biomimetic extracellular matrix properties.

作者信息

Wilson Michelle J, Jiang Yaming, Yañez-Soto Bernardo, Liliensiek Sara, Murphy William L, Nealey Paul F

机构信息

Department of Chemical and Biological Engineering, University of Wisconsin, 1415 Engineering Drive, Madison, Wisconsin 53706.

出版信息

J Vac Sci Technol B Nanotechnol Microelectron. 2012 Nov;30(6):6F903. doi: 10.1116/1.4762842. Epub 2012 Oct 29.

Abstract

Epithelial cells reside on specialized extracellular matrices that provide instructive cues to regulate and support cell function. The authors have previously demonstrated that substrate topography with dimensions similar to the native extracellular matrix (submicrometer and nanoscale features) significantly impacts corneal epithelial proliferation and migration. In this work, synthetic hydrogels were modified with both topographic and biochemical cues, where specified peptide ligands were immobilized within nanopatterned hydrogels. The efficient, systematic study of multiple instructive cues (peptide, peptide concentration, topographic dimensions), however, is contingent on the development of higher throughput platforms. Toward this goal, the authors developed a hydrogel array platform to systematically and rapidly evaluate combinations of two different peptide motifs and a range of nanoscale topographic dimensions. Specifically, distinct functional pegylated peptide ligands, RGD (GGGRGDSP) and AG73 (GRKRLQVQLSIRT), were synthesized for incorporation into an inert hydrogel network. Elastomeric stencils with arrays of millimeter-scale regions were used to spatially confine hydrogel precursor solutions on elastomeric stamps with nanoscale patterns generated by soft lithography. The resulting topographically and peptide-functionalized hydrogel arrays were used to characterize single cell migration. Epithelial cell migration speed and persistence were governed by both the biochemical and topographical cues of the underlying substrate.

摘要

上皮细胞驻留在特殊的细胞外基质上,这些基质提供指导性信号来调节和支持细胞功能。作者此前已证明,尺寸与天然细胞外基质相似(亚微米和纳米级特征)的基质形貌会显著影响角膜上皮细胞的增殖和迁移。在这项工作中,合成水凝胶被同时修饰了形貌和生化信号,特定的肽配体被固定在纳米图案化的水凝胶中。然而,对多种指导性信号(肽、肽浓度、形貌尺寸)进行高效、系统的研究取决于更高通量平台的开发。为实现这一目标,作者开发了一种水凝胶阵列平台,以系统、快速地评估两种不同肽基序和一系列纳米级形貌尺寸的组合。具体而言,合成了不同的功能化聚乙二醇化肽配体RGD(GGGRGDSP)和AG73(GRKRLQVQLSIRT),用于掺入惰性水凝胶网络。带有毫米级区域阵列的弹性模板被用于在通过软光刻产生纳米级图案的弹性印章上空间限制水凝胶前体溶液。所得的具有形貌和肽功能化的水凝胶阵列被用于表征单细胞迁移。上皮细胞的迁移速度和持续性受底层基质的生化和形貌信号共同控制。

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