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在大鼠烧伤创面模型中,长期给予C1抑制剂可改善烧伤创面的局部愈合并减轻心肌炎症。

Prolonged C1 inhibitor administration improves local healing of burn wounds and reduces myocardial inflammation in a rat burn wound model.

作者信息

Begieneman Mark P V, Kubat Bela, Ulrich Magda M W, Hahn Nynke E, Stumpf-Stolker Yvette, Tempelaars Miranda, Middelkoop Esther, Zeerleder Sacha, Wouters Diana, van Ham Marieke S, Niessen Hans W M, Krijnen Paul A J

机构信息

Department of Pathology, VU Medical Center, Amsterdam, The Netherlands.

出版信息

J Burn Care Res. 2012 Jul-Aug;33(4):544-51. doi: 10.1097/BCR.0b013e31823bc2fc.

Abstract

In a previous study, the authors found persistent presence of acute inflammation markers such as C-reactive protein and complement factors locally in burn wounds. This persistence of acute inflammation may not only delay local burn wound healing but also have a systemic effect, for instance on the heart. Here, the effects of C1 esterase inhibitor (C1inh), an inhibitor of complement activation, on burn wound progression and the heart were analyzed in rats. Dorsal full-thickness burn wounds (2 × 4 cm) were induced on female Wistar rats (n = 14). The rats were divided into two groups (n = 7): a control group (just burns) and a C1inh group. C1inh was administered daily intravenously for 14 days. The burn wound, healthy skin from the hind leg (internal control), and the heart were then fixed in formalin. Tissues were analyzed for granulation tissue formation, reepithelialization, amount and type of infiltrating inflammatory cells (granulocytes and macrophages), and inflammatory markers (complement factors C3 and C4). C1inh treatment significantly reduced the amount of granulation tissue and significantly increased reepithelialization. C1inh also significantly reduced macrophage infiltration. Burns induced infiltration of macrophages into the ventricles of the heart and remarkably also into the atria of the heart. This effect could be counteracted by C1inh. These data show that systemic treatment with C1inh acts at different levels resulting in improved healing locally in burn wounds and systemically reduced inflammation in the heart. Therefore, C1inh might be a possible therapeutic intervention for burn wound patients.

摘要

在之前的一项研究中,作者发现烧伤创面局部持续存在急性炎症标志物,如C反应蛋白和补体因子。这种急性炎症的持续存在不仅可能延迟烧伤创面的局部愈合,还可能产生全身影响,比如对心脏的影响。在此,研究人员分析了补体激活抑制剂C1酯酶抑制剂(C1inh)对大鼠烧伤创面进展及心脏的影响。对雌性Wistar大鼠(n = 14)造成背部全层烧伤创面(2×4 cm)。将大鼠分为两组(n = 7):对照组(仅烧伤)和C1inh组。每天静脉注射C1inh,持续14天。然后将烧伤创面、后腿的健康皮肤(内部对照)和心脏固定在福尔马林中。分析组织的肉芽组织形成、再上皮化、浸润性炎症细胞(粒细胞和巨噬细胞)的数量和类型以及炎症标志物(补体因子C3和C4)。C1inh治疗显著减少了肉芽组织的数量,并显著增加了再上皮化。C1inh还显著减少了巨噬细胞浸润。烧伤导致巨噬细胞浸润到心脏的心室,并且明显也浸润到心脏的心房。C1inh可以抵消这种作用。这些数据表明,全身应用C1inh在不同水平发挥作用,从而改善烧伤创面的局部愈合,并在全身减轻心脏炎症。因此,C1inh可能是烧伤创面患者的一种潜在治疗干预措施。

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