转化生长因子- β和碱性成纤维细胞生长因子对糖尿病大鼠创面损伤愈合的刺激作用。

Biotechnology therapeutics Pub Date : 1989-01-01
K N Broadley, A M Aquino, B Hicks, J A Ditesheim, G S McGee, A A Demetriou, S C Woodward, J M Davidson
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引用次数: 0

摘要

在两种伤口修复模型中,比较了重组生长因子对正常和链脲佐菌素诱导的糖尿病大鼠伤口修复率的影响:聚乙烯醇海绵皮下植入和切口损伤。在大鼠背表面做横向切口创口,并用钢线缝合。受伤3天后,大鼠接受单次注射转化生长因子- β或载体直接进入伤口部位。分别于伤后7、14、21天处死动物,测定新鲜创面和福尔马林固定创面的抗拉强度。糖尿病大鼠的伤口修复有预期的缺陷,包括肉芽组织减少、胶原蛋白、蛋白质和DNA数量减少。糖尿病切口的新鲜拉伸强度在第7天为正常的53% (p <或= 0.01),在第21天为正常的29%。固定抗拉强度在第7天为正常水平的41% (p < or = 0.01),到第21天降至正常水平的78% (p < or = 0.01),提示糖尿病创面胶原浓度向正常水平升高,但未成熟。TGF β可使糖尿病大鼠新鲜和固定伤口的抗拉强度适度增加,但未达到未治疗的正常大鼠伤口的水平。海绵中充满肉芽组织,用组织学和生化方法测定肉芽组织的再生率。在海绵中单次注射碱性成纤维细胞生长因子,转化生长因子- β,或仅在海绵中注射培养液,分别在培养后第7天和第9天进行评估。在海绵模型中,bFGF和TGF β均能诱导糖尿病大鼠和正常大鼠肉芽组织积累显著增加。TGF β使糖尿病动物海绵胶原蛋白含量增加136% (p < or = .001),从而使胶原蛋白含量提高到正常对照伤口的水平,同时在第9天刺激正常动物海绵胶原蛋白含量增加49% (p < or = .02)。相比之下,对bFGF的反应主要是海绵蛋白质和DNA含量的增加。这些结果强调了两种细胞因子在伤口修复缺陷条件下加速愈合的不同作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The diabetic rat as an impaired wound healing model: stimulatory effects of transforming growth factor-beta and basic fibroblast growth factor.

Two models of wound repair compared the effect of defined, recombinant growth factors on the rate of wound repair in both normal and streptozotocin-induced diabetic rats: subcutaneous implantation of polyvinyl alcohol sponges and incisional wounding. Transverse incisional wounds were made on the dorsal surface of rats and closed with steel sutures. Three days postwounding the rats received a single injection of either transforming growth factor-beta or vehicle alone directly into the wound site. Animals were sacrificed 7, 14, and 21 days postwounding, and fresh and formalin-fixed wound tensile strength were measured. Diabetic rats had expected defects in wound repair, including decreased granulation tissue and reduced amounts of collagen, protein, and DNA. Fresh tensile strength of the diabetic incisions was 53% of normal on Day 7 (p < or = .01) and 29% of normal on Day 21. Fixed tensile strength was 41% of normal on Day 7 (p < or = .01) and fell to 78% of normal by Day 21 (p < or = .01), suggesting that collagen concentrations of diabetic wounds increased towards normal but did not undergo maturation. TGF beta produced a moderate increase in tensile strength of fresh and fixed wounds of diabetic rats, but not to the levels of wounds in untreated normal rats. Sponges fill with granulation tissue, their reproducible rate of organization being measured by histological and biochemical methods. A single injection into sponges 3 days postimplantation of basic fibroblast growth factor, transforming growth factor-beta, or vehicle only, was evaluated at 7 and 9 days postimplantation. In the sponge model, bFGF and TGF beta were each able to induce significant increases in the accumulation of granulation tissue in both diabetic and normal rats. TGF beta increased the collagen content of sponges by 136% in sponges from diabetic animals (p < or = .001), thereby raising the collagen content to that of normal control wounds, while stimulating a 49% (p < or = .02) increase in sponges from normal animals on Day 9. By contrast, the response to bFGF was predominantly an increase in the protein and DNA content of the sponges. These results emphasize the differential effects of the two cytokines in accelerating healing under conditions of defective wound repair.

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