Thrombin peptide, TP508, stimulates angiogenic responses in animal models of dermal wound healing, in chick chorioallantoic membranes, and in cultured human aortic and microvascular endothelial cells

Andrea M. Norfleet, John S. Bergmann, Darrell H. Carney
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引用次数: 51

Abstract

The α-thrombin peptide, TP508, accelerates the healing of full-thickness wounds in both normal and ischemic skin. In wounds treated with TP508, a pattern of increased vascularization is consistently observed both grossly and microscopically when compared to wounds treated with saline. One possible mechanism by which the peptide accelerates wound healing is by promoting revascularization of granulation tissue at the injured site. To evaluate the angiogenic potential of TP508, the peptide was tested in the chick embryo chorioallantoic membrane (CAM), where it increased the density and size of CAM blood vessels relative to controls. Additionally, TP508 stimulated chemokinesis and chemotaxis in a dose-dependent fashion in cultured human aortic and human microvascular endothelial cells. Taken together, these in vivo and in vitro data support an angiogenic role for TP508 in wound healing. A working model is presented to explain how this 23-amino-acid peptide, which lacks proteolytic activity, is generated during wound healing and contributes to the nonproteolytic functions associated with α-thrombin during tissue repair.

凝血酶肽TP508在动物真皮伤口愈合模型、鸡绒毛膜尿囊膜和培养的人主动脉和微血管内皮细胞中刺激血管生成反应。
α-凝血酶肽TP508可促进正常和缺血皮肤全层创面愈合。在用TP508处理的伤口中,与用生理盐水处理的伤口相比,在肉眼和显微镜下都一致观察到血管化增加的模式。肽加速伤口愈合的一个可能机制是通过促进受伤部位肉芽组织的血运重建。为了评估TP508的血管生成潜能,我们在鸡胚绒毛尿囊膜(CAM)中测试了TP508肽,与对照组相比,它增加了CAM血管的密度和大小。此外,TP508在培养的人主动脉和微血管内皮细胞中以剂量依赖性的方式刺激趋化运动和趋化性。综上所述,这些体内和体外数据支持TP508在伤口愈合中的血管生成作用。本文提出了一个工作模型来解释这种缺乏蛋白水解活性的23个氨基酸肽是如何在伤口愈合过程中产生的,并有助于在组织修复过程中与α-凝血酶相关的非蛋白水解功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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