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Proteolytic signatures define unique thrombin-derived peptides present in human wound fluid in vivo

机译:蛋白水解特征定义了人体伤口液中存在的独特的凝血酶衍生肽

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摘要

The disease burden of failing skin repair and non-healing ulcers is extensive. There is an unmet need for new diagnostic approaches to better predict healing activity and wound infection. Uncontrolled and excessive protease activity, of endogenous or bacterial origin, has been described as a major contributor to wound healing impairments. Proteolytic peptide patterns could therefore correlate and “report” healing activity and infection. This work describes a proof of principle delineating a strategy by which peptides from a selected protein, human thrombin, are detected and attributed to proteolytic actions. With a particular focus on thrombin-derived C-terminal peptides (TCP), we show that distinct peptide patterns are generated in vitro by the human S1 peptidases human neutrophil elastase and cathepsin G, and the bacterial M4 peptidases Pseudomonas aeruginosa elastase and Staphylococcus aureus aureolysin, respectively. Corresponding peptide sequences were identified in wound fluids from acute and non-healing ulcers, and notably, one peptide, FYT21 (FYTHVFRLKKWIQKVIDQFGE), was only present in wound fluid from non-healing ulcers colonized by P. aeruginosa and S. aureus. Our result is a proof of principle pointing at the possibility of defining peptide biomarkers reporting distinct proteolytic activities, of potential implication for improved diagnosis of wound healing and infection.
机译:皮肤修复失败和溃疡不愈的疾病负担是广泛的。对新的诊断方法的需求未得到满足,以更好地预测愈合活性和伤口感染。已经描述了内源性或细菌性来源的不受控制的和过度的蛋白酶活性,是导致伤口愈合障碍的主要因素。因此,蛋白水解肽的模式可以关联并“报告”愈合活性和感染。这项工作描述了原理证明,描绘了一种策略,通过该策略可以检测到来自选定蛋白质(人类凝血酶)的肽并将其归因于蛋白水解作用。我们特别关注凝血酶衍生的C末端肽(TCP),我们显示了人S1肽酶,人类嗜中性粒细胞弹性蛋白酶和组织蛋白酶G,以及细菌M4肽酶铜绿假单胞菌弹性蛋白酶和金黄色葡萄球菌金黄色葡萄球菌溶血素在体外产生了独特的肽模式, 分别。在急性和非愈合性溃疡的伤口液中鉴定出相应的肽序列,值得注意的是,一种肽FYT21(FYTHVFRLKKWIQKVIDQFGE)仅存在于铜绿假单胞菌和金黄色葡萄球菌定植的非愈合性溃疡的伤口液中。我们的结果是原理证明,指出了定义报告具有独特蛋白水解活性的肽生物标志物的可能性,这对改善伤口愈合和感染的诊断具有潜在意义。

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