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Focused Screening of ECM-Selective Adhesion Peptides on Cellulose-Bound Peptide Microarrays

机译:在纤维素结合肽微阵列上对ECM选择性粘附肽的集中筛选

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摘要

The coating of surfaces with bio-functional proteins is a promising strategy for the creation of highly biocompatible medical implants. Bio-functional proteins from the extracellular matrix (ECM) provide effective surface functions for controlling cellular behavior. We have previously screened bio-functional tripeptides for feasibility of mass production with the aim of identifying those that are medically useful, such as cell-selective peptides. In this work, we focused on the screening of tripeptides that selectively accumulate collagen type IV (Col IV), an ECM protein that accelerates the re-endothelialization of medical implants. A SPOT peptide microarray was selected for screening owing to its unique cellulose membrane platform, which can mimic fibrous scaffolds used in regenerative medicine. However, since the library size on the SPOT microarray was limited, physicochemical clustering was used to provide broader variation than that of random peptide selection. Using the custom focused microarray of 500 selected peptides, we assayed the relative binding rates of tripeptides to Col IV, collagen type I (Col I), and albumin. We discovered a cluster of Col IV-selective adhesion peptides that exhibit bio-safety with endothelial cells. The results from this study can be used to improve the screening of regeneration-enhancing peptides.
机译:用生物功能蛋白包被表面是创建高度生物相容性医学植入物的有前途的策略。来自细胞外基质(ECM)的生物功能蛋白为控制细胞行为提供了有效的表面功能。我们先前已经针对大规模生产的可行性筛选了生物功能三肽,目的是鉴定可用于医学的三肽,例如细胞选择性肽。在这项工作中,我们专注于筛选选择性积聚IV型胶原(Col IV)的三肽,ECM蛋白可加速医用植入物的再内皮化。由于SPOT肽微阵列具有独特的纤维素膜平台,因此可以模拟再生医学中使用的纤维支架,因此选择进行筛选。但是,由于SPOT微阵列上的文库大小有限,因此使用理化聚类比随机肽选择提供了更大的变异。使用500个选定肽的定制聚焦微阵列,我们测定了三肽与Col IV,I型胶原(Col I)和白蛋白的相对结合率。我们发现了一组Col IV选择性粘附肽,它们对内皮细胞具有生物安全性。这项研究的结果可用于改善再生增强肽的筛选。

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