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血小板衍生生长因子和重组c-sis基因同源二聚体蛋白增强体内切口伤口愈合。

In vivo incisional wound healing augmented by platelet-derived growth factor and recombinant c-sis gene homodimeric proteins.

作者信息

Pierce G F, Mustoe T A, Senior R M, Reed J, Griffin G L, Thomason A, Deuel T F

机构信息

Department of Medicine, Jewish Hospital, Washington University Medical Center, St. Louis, Missouri 63110.

出版信息

J Exp Med. 1988 Mar 1;167(3):974-87. doi: 10.1084/jem.167.3.974.

Abstract

Human platelet-derived growth factor (hPDGF) is likely to be important in stimulating tissue repair, based upon its in vivo chemotactic and stimulatory activities for inflammatory cells and fibroblasts and upon the presence of PDGF and related proteins in platelets, macrophages, and activated fibroblasts, cell types that make up the milieu of the healing wound. Recombinant human c-sis (rPDGF-B), homodimers of the B chain of PDGF, were compared with hPDGF in vitro. rPDGF-B was immunologically similar to hPDGF and, at identical concentrations, similar to hPDGF in stimulating fibroblast mitogenesis and chemotaxis of polymorphonuclear leukocytes, monocytes, and fibroblasts. Purified hPDGF and rPDGF-B were also tested in vivo for potency in a model of tissue repair using a linear incision wound through rat dermis. A single application of hPDGF or rPDGF-B (2-20 micrograms/wound) in a slow release vehicle at the time of wounding resulted in a dose-dependent, statistically highly significant increase of breaking strength of treated wounds. Wound healing in animals treated with rPDGF-B was 170% stronger and accelerated by 2 d during the first week over control wounds and by 4-6 d over the next 2 wk. Histologic evaluation of growth factor-treated wounds correlated the in vitro chemotactic activity and the accelerated healing of wounds with a striking inflammatory cell infiltrate early after wounding, markedly increased formation of granulation tissue by 4-d, and increased fibrosis by 14 d in comparison to control wounds. The results thus demonstrate that rPDGF-B is fully active in in vitro tests of mitogenesis and chemotaxis and, for the first time, demonstrate directly that PDGF significantly advances wound healing in incisional wounds of experimental animals.

摘要

基于人血小板衍生生长因子(hPDGF)对炎症细胞和成纤维细胞的体内趋化和刺激活性,以及血小板、巨噬细胞和活化成纤维细胞(构成愈合伤口环境的细胞类型)中存在PDGF及相关蛋白,hPDGF可能在刺激组织修复中起重要作用。在体外将重组人c-sis(rPDGF-B,PDGF B链的同二聚体)与hPDGF进行比较。rPDGF-B在免疫学上与hPDGF相似,在相同浓度下,在刺激成纤维细胞有丝分裂以及多形核白细胞、单核细胞和成纤维细胞的趋化性方面与hPDGF相似。还在体内使用大鼠真皮线性切口伤口的组织修复模型测试了纯化的hPDGF和rPDGF-B的效力。在伤口形成时,将hPDGF或rPDGF-B(2 - 20微克/伤口)单次应用于缓释载体中,导致处理伤口的抗张强度呈剂量依赖性、统计学上高度显著增加。用rPDGF-B处理的动物伤口愈合比对照伤口在第一周时强170%且加速2天,在接下来的2周内加速4 - 6天。对生长因子处理伤口的组织学评估将体外趋化活性和伤口加速愈合与伤口早期显著的炎症细胞浸润、4天时肉芽组织形成明显增加以及与对照伤口相比14天时纤维化增加相关联。因此,结果表明rPDGF-B在有丝分裂和趋化性的体外测试中具有完全活性,并且首次直接证明PDGF显著促进实验动物切口伤口的愈合。

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