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增强巨噬细胞功能对早期伤口愈合的影响。

Effect of enhanced macrophage function on early wound healing.

作者信息

Browder W, Williams D, Lucore P, Pretus H, Jones E, McNamee R

机构信息

Department of Surgery, Tulane University School of Medicine, New Orleans, LA 70112.

出版信息

Surgery. 1988 Aug;104(2):224-30.

PMID:3261048
Abstract

Although the macrophage is important to wound healing, research has focused on its relationship to fibroblast and collagen synthesis. This study was designed to assess effects of enhanced macrophage function on early wound healing, before established collagen synthesis. Sprague-Dawley rats had dorsal incisions after one of three treatment regimens: (1) saline solution, 0.5 ml administered intravenously, (2) intravenous glucan, a macrophage stimulant, 20 mg; (3) topical glucan, 20 mg. Intravenous therapy was administered 24 hours before and after incision. Breaking strength was significantly increased (p less than 0.01) by both intravenous glucan (49.8 +/- 5.5 gm) and topical glucan (59.7 +/- 5.6 gm) on the fourth day after incision, compared with controls (22.0 +/- 2.6 gm). Similar results occurred on the seventh day after incision. Although formalin fixation significantly enhanced breaking strength in fresh control wounds (22.0 +/- 2.6 vs 39.5 +/- 2.2 gm), no increase occurred in wounds treated with intravenous glucan (49.8 +/- 5.0 vs 55.3 +/- 6.4 gm), indicating maximal cross-linking of collagen. Collagen synthesis, reflected by tritiated proline uptake, was no different in control versus glucan groups. Supernatants from control or glucan-activated macrophages were injected intraperitoneally or applied topically in the rat model. Activated supernatant, both intraperitoneal and topical, resulted in increased breaking strength on the fourth day after incision. Formalin fixation did not increase breaking strength in the activated supernatant groups. We conclude that enhanced macrophage function increases early wound breaking strength. This effect appears unrelated to collagen synthesis but may be related to increased cross-linking of collagen. Similar effects are seen with activated macrophage secretory products administered intraperitoneally or topically.

摘要

尽管巨噬细胞对伤口愈合很重要,但研究主要集中在其与成纤维细胞和胶原蛋白合成的关系上。本研究旨在评估在胶原蛋白合成确立之前,增强巨噬细胞功能对早期伤口愈合的影响。将Sprague-Dawley大鼠分为三组,分别接受以下三种处理方案之一后进行背部切口:(1)静脉注射0.5 ml生理盐水;(2)静脉注射20 mg巨噬细胞刺激剂葡聚糖;(3)局部应用20 mg葡聚糖。在切口前后24小时进行静脉治疗。与对照组(22.0±2.6 g)相比,切口后第四天静脉注射葡聚糖组(49.8±5.5 g)和局部应用葡聚糖组(59.7±5.6 g)的断裂强度均显著增加(p<0.01)。切口后第七天出现类似结果。尽管福尔马林固定显著提高了新鲜对照伤口的断裂强度(22.0±2.6 g对39.5±2.2 g),但静脉注射葡聚糖治疗的伤口未出现增加(49.8±5.0 g对55.3±6.4 g),表明胶原蛋白已达到最大交联。以氚标记脯氨酸摄取量反映的胶原蛋白合成,在对照组和葡聚糖组之间没有差异。将对照组或葡聚糖激活的巨噬细胞的上清液腹腔内注射或局部应用于大鼠模型。腹腔内和局部应用激活的上清液,均导致切口后第四天断裂强度增加。福尔马林固定未增加激活上清液组的断裂强度。我们得出结论,增强巨噬细胞功能可提高早期伤口的断裂强度。这种作用似乎与胶原蛋白合成无关,但可能与胶原蛋白交联增加有关。腹腔内或局部应用激活的巨噬细胞分泌产物也观察到类似效果。

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