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伤口愈合的当前概念:生长因子与巨噬细胞的相互作用。

Current concepts in wound healing: growth factor and macrophage interaction.

作者信息

Cromack D T, Porras-Reyes B, Mustoe T A

机构信息

Department of Surgery, Barnes Hospital, St. Louis, MO 63110.

出版信息

J Trauma. 1990 Dec;30(12 Suppl):S129-33. doi: 10.1097/00005373-199012001-00026.

Abstract

Growth factors are potent wound healing promoters which accelerate incisional wound repair by distinct mechanisms. Transforming growth factor-beta (TGF-beta), a chemotactic factor, increases synthesis of extracellular matrix and stimulates granulation tissue. We demonstrated that a single topical dose of TGF-beta increased the wound breaking strength in normal models of tissue repair as well as in models of impaired wound repair, characterized by severe monocytopenia. PDGF, a chemotactic agent for inflammatory cells, with mitogenic activity, activates monocytes and stimulates collagen production, significantly increased the wound breaking strength with effects that lasted for up to 47 days. In contrast to TGF-beta, PDGF was only active in normal models of wound healing and its effects were dependent upon the presence of macrophages. PAF is a glycerophospholipid which chemotaxes and activates macrophages, but differs from growth factors in lacking mitogenic activity. A single topical dose of PAF significantly increased the wound breaking strength and promoted macrophage migration.

摘要

生长因子是强大的伤口愈合促进剂,可通过不同机制加速切口伤口修复。转化生长因子-β(TGF-β)是一种趋化因子,可增加细胞外基质的合成并刺激肉芽组织生长。我们证明,在正常组织修复模型以及以严重单核细胞减少为特征的伤口修复受损模型中,单次局部应用TGF-β均可提高伤口抗张强度。血小板衍生生长因子(PDGF)是一种炎症细胞趋化剂,具有促有丝分裂活性,可激活单核细胞并刺激胶原蛋白生成,显著提高伤口抗张强度,其作用可持续长达47天。与TGF-β不同,PDGF仅在正常伤口愈合模型中具有活性,其作用依赖于巨噬细胞的存在。血小板活化因子(PAF)是一种甘油磷脂,可趋化并激活巨噬细胞,但与生长因子不同,它缺乏促有丝分裂活性。单次局部应用PAF可显著提高伤口抗张强度并促进巨噬细胞迁移。

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