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A systematic methodology for proteome-wide identification of peptides inhibiting the proliferation and migration of endothelial cells

机译:蛋白质组学范围内鉴定抑制内皮细胞增殖和迁移的多肽的系统方法

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摘要

We introduce a systematic computational methodology based on bioinformatics that has enabled us to identify and classify >120 endogenous peptide inhibitors of endothelial cell proliferation and migration. These peptides are derived from members of the type IV collagen, thrombospondin, and CXC chemokine protein families, as well as somatotropin hormones, serpins, and various kringle-containing proteins. Their activity in suppressing the proliferation and migration of endothelial cells in vitro provides proof of principle for the validity of this computational method. Interestingly, some of the peptides are derived from proteins known to be proangiogenic. By performing receptor neutralization studies, we have identified receptors to which these peptides bind. On the basis of this receptor-binding information, we evaluated several examples of peptide-based combinatorial screening strategies. In some cases, this combinatorial screening identified strong synergism between peptides. The current work provides a guideline for a computational-based peptidomics approach for the discovery of endogenous bioactive peptides.
机译:我们介绍了一种基于生物信息学的系统计算方法,该方法使我们能够识别和分类> 120种内皮细胞增殖和迁移的内源性肽抑制剂。这些肽衍生自IV型胶原蛋白,血小板反应蛋白和CXC趋化因子蛋白家族的成员,以及生长激素激素,丝氨酸蛋白酶抑制剂和各种含环蛋白。它们在体外抑制内皮细胞增殖和迁移中的活性为该计算方法的有效性提供了原理证明。有趣的是,某些肽衍生自已知具有促血管生成作用的蛋白质。通过进行受体中和研究,我们确定了这些肽结合的受体。在此受体结合信息的基础上,我们评估了基于肽的组合筛选策略的几个例子。在某些情况下,这种组合筛选确定了肽之间的强协同作用。当前的工作为发现内源性生物活性肽的基于计算的肽组学方法提供了指南。

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