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用重组血小板衍生生长因子BB治疗慢性压疮时的组织修复过程

Tissue repair processes in healing chronic pressure ulcers treated with recombinant platelet-derived growth factor BB.

作者信息

Pierce G F, Tarpley J E, Allman R M, Goode P S, Serdar C M, Morris B, Mustoe T A, Vande Berg J

机构信息

Department of Experimental Pathology, Amgen Inc., Thousand Oaks, California.

出版信息

Am J Pathol. 1994 Dec;145(6):1399-410.

Abstract

Cellular and molecular mechanisms responsible for the observed vulnerary effects of recombinant human platelet-derived growth factor BB (rP-DGF-BB) in man have not been elucidated. In a double-blinded trial, patients having chronic pressure ulcers were treated topically with either rPDGF-BB or placebo for 28 days. To explore how rPDGF-BB may induce chronic wounds to heal, biopsies were taken from the ulcers of a cohort of 20 patients from the trial and evaluated in a blinded fashion by light microscopy for 1), fibroblast content, 2) neovessel formation, and 3), collagen deposition. Electron microscopy also was used to assess fibroblast activation and collagen deposition. Before initiation of therapy most wounds had few fibroblasts and most of those present were not activated. When mean scores for the total active treatment phase (days 8, 15, and 29) for rPDGF-BB-treated ulcers were compared with the scores for placebo-treated ulcers, fibroblast content was significantly higher for the rPDGF-BB-treated ulcers (P = 0.03, Kruskal-Wallis test). More significant differences in fibroblast and neovessel content were observed when six nonhealing wounds were eliminated from the analysis (three placebo, three treatment). Thus, in all healing wounds, rPDGF-BB therapy significantly increased fibroblast (P = 0.0007) and neovessel (P = 0.02) content. These results were correlated with increased collagen fibrillogenesis by fibroblasts from healing rPDGF-BB-treated wounds, as assessed by intracellular procollagen type I immunostaining, and by electron microscopy, and were concordant with clinical measurements (eg, area of ulcer opening and ulcer volume) which showed greater healing in rPDGF-BB-treated wounds. These results suggest induction of fibroblast proliferation and differentiation is one mechanism by which rPDGF-BB can accelerate wound healing and that rPDGF-BB can augment healing responses within a majority of, but not all, nonhealing chronic pressure ulcers in man.

摘要

重组人血小板衍生生长因子BB(rP-DGF-BB)在人体中所观察到的促进愈合作用的细胞和分子机制尚未阐明。在一项双盲试验中,患有慢性压疮的患者局部使用rPDGF-BB或安慰剂治疗28天。为探究rPDGF-BB如何诱导慢性伤口愈合,从该试验的20名患者的溃疡处取活检组织,并通过光学显微镜以盲法评估:1)成纤维细胞含量;2)新血管形成;3)胶原沉积。还使用电子显微镜评估成纤维细胞活化和胶原沉积。在治疗开始前,大多数伤口的成纤维细胞很少,且大多数现存的成纤维细胞未被激活。将rPDGF-BB治疗溃疡的整个活性治疗阶段(第8、15和29天)的平均得分与安慰剂治疗溃疡的得分进行比较时,rPDGF-BB治疗的溃疡的成纤维细胞含量显著更高(P = 0.03,Kruskal-Wallis检验)。当从分析中排除六个未愈合伤口(三个安慰剂组,三个治疗组)时,观察到成纤维细胞和新血管含量的差异更显著。因此,在所有愈合的伤口中,rPDGF-BB治疗显著增加了成纤维细胞(P = 0.0007)和新血管(P = 0.02)含量。这些结果与通过细胞内I型前胶原免疫染色和电子显微镜评估的来自rPDGF-BB治疗愈合伤口的成纤维细胞增加的胶原纤维形成相关,并且与临床测量结果(例如溃疡开口面积和溃疡体积)一致,这些结果显示rPDGF-BB治疗的伤口愈合更好。这些结果表明,诱导成纤维细胞增殖和分化是rPDGF-BB加速伤口愈合的一种机制,并且rPDGF-BB可以增强大多数(但不是全部)人类非愈合慢性压疮的愈合反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f0d/1887508/8d09f0ee4f2f/amjpathol00060-0163-a.jpg

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