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战斗伤口愈合中的炎症生物标志物。

Inflammatory biomarkers in combat wound healing.

机构信息

Department of Regenerative Medicine, Combat Casualty Care, Naval Medical Research Center, Silver Spring, MD 20910, USA.

出版信息

Ann Surg. 2009 Dec;250(6):1002-7. doi: 10.1097/sla.0b013e3181b248d9.

Abstract

BACKGROUND

Modern war ballistics and blast injuries inflict devastating extremity injuries, violating soft tissue, bone, and neurovascular structures. Despite advances in complex wound management, appropriate timing of war wound closure remains subjective. In addition, the pathophysiology of acute wound failure is poorly defined.

METHODS

Patients with penetrating extremity wounds sustained during combat were prospectively studied and followed for 30 days after definitive wound closure. The primary outcome was wound healing. Wound dehiscence was defined as spontaneous partial or complete wound disruption after closure. Serum, wound effluent, and wound bed tissue biopsy were collected at each surgical wound debridement. Serum and wound effluent were analyzed with a multiplex array of 22 cytokines and chemokines, and wound tissue for corresponding gene transcript expression.

RESULTS

Fifty-two penetrating extremity war wounds in 33 male patients were investigated. Nine (17%) wounds dehisced. Concomitant vascular injury, increased wound size, and higher injury severity score correlated with wound dehiscence. Both serum and wound effluent cytokine and chemokine protein profiles were statistically associated with healing outcome at various time points. Wound biopsy gene transcript expression demonstrated increased tissue inflammation associated with wound failure. Multiple protein and gene transcript biomarkers predictive of wound healing were identified.

CONCLUSIONS

The cytokine and chemokine protein and gene transcript expression patterns demonstrate a condition of inflammatory dysregulation associated with war wound failure. A molecular biomarker panel may predict combat wound healing outcome and warrants prospective validation.

摘要

背景

现代战争中的弹道和爆炸伤会导致毁灭性的四肢损伤,破坏软组织、骨骼和神经血管结构。尽管在复杂伤口管理方面取得了进展,但战争伤口闭合的适当时机仍然是主观的。此外,急性伤口失败的病理生理学定义不明确。

方法

前瞻性研究了在战斗中遭受穿透性四肢伤口的患者,并在确定性伤口闭合后随访 30 天。主要结果是伤口愈合。伤口裂开定义为闭合后自发的部分或完全伤口破裂。每次手术清创时都采集血清、伤口渗出液和伤口床组织活检。使用 22 种细胞因子和趋化因子的多重微阵列分析血清和伤口渗出液,并分析伤口组织的相应基因转录表达。

结果

研究了 33 名男性患者的 52 个穿透性四肢战伤。9 个(17%)伤口裂开。伴发的血管损伤、伤口增大和更高的损伤严重程度评分与伤口裂开相关。血清和伤口渗出液细胞因子和趋化因子蛋白谱在不同时间点与愈合结果均具有统计学相关性。伤口活检基因转录表达显示与伤口失败相关的组织炎症增加。确定了多个预测伤口愈合的蛋白质和基因转录生物标志物。

结论

细胞因子和趋化因子的蛋白和基因转录表达模式表明与战争伤口失败相关的炎症失调状态。分子生物标志物谱可能预测战斗伤口愈合结果,值得进一步前瞻性验证。

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