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通过微阵列技术以及测量CD18缺陷小鼠受伤皮肤中的新血管形成来描绘多形核中性粒细胞的促血管生成能力。

The proangiogenic capacity of polymorphonuclear neutrophils delineated by microarray technique and by measurement of neovascularization in wounded skin of CD18-deficient mice.

作者信息

Schruefer Ruth, Sulyok Silke, Schymeinsky Jurgen, Peters Thorsten, Scharffetter-Kochanek Karin, Walzog Barbara

机构信息

Department of Physiology, Ludwig Maximilians University, Munich, Germany.

出版信息

J Vasc Res. 2006;43(1):1-11. doi: 10.1159/000088975. Epub 2005 Oct 14.

DOI:10.1159/000088975
PMID:16227701
Abstract

Growing evidence supports the concept that polymorphonuclear neutrophils (PMN) are critically involved in inflammation-mediated angiogenesis which is important for wound healing and repair. We employed an oligonucleotide microarray technique to gain further insight into the molecular mechanisms underlying the proangiogenic potential of human PMN. In addition to 18 known angiogenesis-relevant genes, we detected the expression of 10 novel genes, namely midkine, erb-B2, ets-1, transforming growth factor receptor-beta2 and -beta3, thrombospondin, tissue inhibitor of metalloproteinase 2, ephrin A2, ephrin B2 and restin in human PMN freshly isolated from the circulation. Gene expression was confirmed by the RT-PCR technique. In vivo evidence for the role of PMN in neovascularization was provided by studying neovascularization in a skin model of wound healing using CD18-deficient mice which lack PMN infiltration to sites of lesion. In CD18-deficient animals, neovascularization was found to be significantly compromised when compared with wild-type control animals which showed profound neovascularization within the granulation tissue during the wound healing process. Thus, PMN infiltration seems to facilitate inflammation-mediated angiogenesis which may be a consequence of the broad spectrum of proangiogenic factors expressed by these cells.

摘要

越来越多的证据支持多形核中性粒细胞(PMN)在炎症介导的血管生成中起关键作用,而炎症介导的血管生成对伤口愈合和修复很重要。我们采用寡核苷酸微阵列技术,以进一步深入了解人PMN促血管生成潜力的分子机制。除了18个已知的与血管生成相关的基因外,我们还检测到10个新基因的表达,即中期因子、erb-B2、ets-1、转化生长因子受体-β2和-β3、血小板反应蛋白、金属蛋白酶组织抑制剂2、ephrin A2、ephrin B2和restin,这些基因存在于从循环中新鲜分离的人PMN中。基因表达通过RT-PCR技术得到证实。通过使用缺乏PMN浸润到损伤部位的CD18缺陷小鼠,在伤口愈合的皮肤模型中研究新生血管形成,为PMN在新生血管形成中的作用提供了体内证据。与野生型对照动物相比,在CD18缺陷动物中,发现新生血管形成明显受损,野生型对照动物在伤口愈合过程中在肉芽组织内显示出明显的新生血管形成。因此,PMN浸润似乎促进了炎症介导的血管生成,这可能是这些细胞表达的广泛促血管生成因子的结果。

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