Journal
SURGERY
Volume 130, Issue 5, Pages 826-833Publisher
MOSBY, INC
DOI: 10.1067/msy.2001.116669
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Funding
- NCI NIH HHS [T32CA68971] Funding Source: Medline
- NIDDK NIH HHS [R01 DK50201] Funding Source: Medline
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Background. Cyclooxygenase-2 (Cox-2), the inducible form of Cox, is a rate-limiting enzyme in the synthesis of Prostaglandins (PGs). Prostaglandin E-2 (PGE(2)) and other eicosanoids possess immunosuppressive properties. Previously, traumatic injury was found to stimulate the synthesis of PGs and cause immune ( dysfunction. In. this study a murine model was used to determine the effect of trauma on the expression of Cox-2 in macrophages and to elucidate the role of Cox-2 in trauma-induced immune dysfunction. Methods. Mice were randomized to control or trauma (femur fracture plus 40% blood volume hemorrhage) groups. One, 4, and 7 days after injury, splenic macrophages were isolated and assayed for expression of Cox-2 and production of PGF(2). In addition, the effect of pharmacologically inhibiting Cox-2 or knocking out the Cox-2 gene on trauma-induced suppression of splenocyte mitogenesis was determined. Results. Trauma led to increased expression of Cox-2, enhanced synthesis of PGE(2), and suppressed splenocyte mitogenesis. Both pharmacologic inhibition and genetic deletion of Cox-2 abrogated trauma-mediated suppression of splenocyte mitogenesis. Conclusions. These experiments link trauma-induced increases in Cox-2 expression and PGE(2) production to reduced immune function. Cox-2 represents a potential pharmacologic target to Prevent or reverse trauma-induced immunosuppression.
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