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受损组织血管系统中的分子变化。

Molecular changes in the vasculature of injured tissues.

作者信息

Järvinen Tero A H, Ruoslahti Erkki

机构信息

Cancer Research Center, Burnham Institute for Medical Research, La Jolla, CA, USA.

出版信息

Am J Pathol. 2007 Aug;171(2):702-11. doi: 10.2353/ajpath.2007.061251. Epub 2007 Jun 28.

Abstract

We have explored molecular specialization of the vasculature of regenerating wound tissue in the skin and tendons to identify a different repertoire of markers from that obtained by studying tumor vasculature. We screened a phage-displayed peptide library for peptides that home to wounds in mice and identified two peptides that selectively target phage to skin and tendon wounds: CARSKNKDC (CAR) and CRKDKC (CRK). CAR is homologous to heparin-binding sites in various proteins and binds to cell surface heparan sulfate and heparin. CRK is similar to a segment in thrombospondin type 1 repeat. Intravenously injected CAR and CRK phage, as well as fluorescein-labeled CAR and CRK peptides, selectively accumulated at wound sites, where they partially co-localized with blood vessels. The CAR peptide showed a preference for early stages of wound healing, whereas the CRK favored wounds at later stages of healing. The CAR peptide was internalized into the target cells and delivered the fluorescent label into the cell nuclei. These results identify new molecular markers in wound tissues and show that the expression of these markers in wound vasculature changes as healing progresses. The peptides recognizing these markers may be useful in delivering treatments into regenerating tissues.

摘要

我们已经探索了皮肤和肌腱中再生伤口组织脉管系统的分子特化,以确定与通过研究肿瘤脉管系统所获得的不同的标记物库。我们筛选了一个噬菌体展示肽库,寻找能归巢到小鼠伤口的肽,并鉴定出两种能将噬菌体选择性靶向皮肤和肌腱伤口的肽:CARSKNKDC(CAR)和CRKDKC(CRK)。CAR与多种蛋白质中的肝素结合位点同源,并与细胞表面硫酸乙酰肝素和肝素结合。CRK类似于血小板反应蛋白1型重复序列中的一个片段。静脉注射的CAR和CRK噬菌体,以及荧光素标记的CAR和CRK肽,选择性地在伤口部位聚集,在那里它们部分与血管共定位。CAR肽对伤口愈合的早期阶段表现出偏好,而CRK则更倾向于愈合后期的伤口。CAR肽被内化到靶细胞中,并将荧光标记物递送到细胞核中。这些结果确定了伤口组织中的新分子标记物,并表明这些标记物在伤口脉管系统中的表达随着愈合进程而变化。识别这些标记物的肽可能有助于将治疗药物递送到再生组织中。

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