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小动物模型中挤压综合征及再灌注间隔后的全身和组织学损伤特征

Characterization of systemic and histologic injury after crush syndrome and intervals of reperfusion in a small animal model.

作者信息

Murata Isamu, Ooi Kazuya, Sasaki Hiromi, Kimura Soichiro, Ohtake Kazuo, Ueda Hideo, Uchida Hiroyuki, Yasui Norikiyo, Tsutsui Yasuhiro, Yoshizawa Naoya, Hirotsu Ichiro, Morimoto Yasunori, Kobayashi Jun

机构信息

Division of Pathophysiology, Department of Clinical Dietetics and Human Nutrition, Faculty of Pharmaceutical Science, Josai University, Saitama, Japan.

出版信息

J Trauma. 2011 Jun;70(6):1453-63. doi: 10.1097/TA.0b013e31820ca00a.

Abstract

BACKGROUND

Prolonged compression of limb muscles and subsequent decompression are important in the development of crush syndrome (CS). We applied a simple rubber tourniquet to rat hind limbs to create a CS model.

METHODS

Anesthetized rats were subjected to bilateral hind limb compression for 5 hours followed by decompression and reperfusion for 0 hour, 1 hour, 3 hours, and 24 hours under monitoring of arterial blood pressure and electrocardiography. Blood and tissue samples were collected for histology, biochemical analysis, and tissue myeloperoxidase activity assessment.

RESULTS

The survival rates of the CS-model groups remained at 100% until 3 hours, however, dropped to 25% at 24 hours after reperfusion mainly because of hyperkalemia and consequent hypotension observed at 1 hour and deteriorated at 3 hours after reperfusion. Rhabdomyolysis evaluated by circulating and histologic markers of injury was found as early as 1 hour and more marked at 3 hours, resulting in impaired renal function 24 hours after reperfusion. Myeloperoxidase activities increased with incremental periods after reperfusion not only in injured limb muscles but also in kidney and lung, suggesting an abnormal interaction between the vascular endothelium and circulating leukocytes after rhabdomyolysis, possibly causing subsequent multiple organ dysfunction frequently encountered in CS.

CONCLUSION

The findings from this study demonstrate the feasibility of a novel small animal model of extremity crush injury. By using this model, the impact of incremental periods of reperfusion on mortality and remote organ dysfunctions can be characterized. Future studies are necessary to better define a threshold for this injury pattern and the impact of other factors underlying this syndrome.

摘要

背景

肢体肌肉的长时间压迫及随后的减压在挤压综合征(CS)的发生发展中起重要作用。我们应用一种简单的橡胶止血带对大鼠后肢进行处理以建立CS模型。

方法

对麻醉后的大鼠双侧后肢进行5小时压迫,随后在动脉血压和心电图监测下分别进行0小时、1小时、3小时和24小时的减压及再灌注。采集血液和组织样本进行组织学、生化分析以及组织髓过氧化物酶活性评估。

结果

CS模型组的存活率在3小时前一直保持在100%,然而,再灌注24小时时降至25%,主要原因是再灌注1小时时出现高钾血症及随之而来的低血压,并在3小时时恶化。通过循环和组织损伤标志物评估的横纹肌溶解在1小时时就已出现,3小时时更为明显,导致再灌注24小时后肾功能受损。髓过氧化物酶活性在再灌注后的不同时间段均增加,不仅在受伤的肢体肌肉中,在肾脏和肺中也是如此,提示横纹肌溶解后血管内皮细胞与循环白细胞之间存在异常相互作用,可能导致CS中常见的后续多器官功能障碍。

结论

本研究结果证明了一种新型的小动物肢体挤压伤模型的可行性。通过使用该模型,可以明确再灌注不同时间段对死亡率和远处器官功能障碍的影响。未来有必要开展进一步研究,以更好地确定这种损伤模式的阈值以及该综合征其他潜在因素的影响。

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