Antiinflammatory effects of soluble complement receptor type 1 promote rapid recovery of ischemia/reperfusion injury in rat small intestine

被引：55

作者：

Eror, AT ^{[1
]}

Stojadinovic, A

Starnes, BW

Makrides, SC

Tsokos, GC

Shea-Donohue, T

机构：

[1] Walter Reed Army Med Ctr, Dept Surg, Washington, DC 20307 USA

[2] Walter Reed Army Med Ctr, Walter Reed Army Inst Res, Dept Clin Physiol, Washington, DC 20307 USA

[3] PRAECIS Pharmaceut Inc, Dept Cell Biol, Cambridge, MA USA

[4] Uniformed Serv Univ Hlth Sci, Dept Med, Bethesda, MD 20814 USA

来源：

CLINICAL IMMUNOLOGY | 1999年 / 90卷 / 02期

关键词：

intestine; ischemia/reperfusion; neutrophil; leukotriene B-4; soluble complement receptor type 1;

D O I：

10.1006/clim.1998.4635

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

We examined the effect of soluble complement receptor type I (sCR1) on mucosal injury and inflammation in a rat model of ischemia/reperfusion. Groups of vehicle- and sCR1-treated rats underwent 30 min of mesenteric ischemia followed by 60 or 120 min of reperfusion. When compared to vehicle-treated rats, treatment with sCR1 (12 mg/kg) prior to 120 min of reperfusion significantly reduced mucosal injury, neutrophil infiltration, leukotriene B-4 production, and restored villus height to control levels. The protective effect of sCR1 evident at 120 min of reperfusion was not observed at 60 min of reperfusion despite rapid inactivation of complement. These data suggest that complement inhibition minimized mucosal disruption by facilitating mucosal restitution or interrupting the inflammatory process. Delayed administration of sCR1 for 30 or 60 min into the reperfusion period progressively reduced the protection. sCR1-mediated rapid recovery of rat intestine after ischemia/reperfusion underscores the fundamental role of complement activation in neutrophil-mediated tissue injury.

引用

页码：266 / 275

页数：10

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