Effect of interleukin-15 on depressed splenic dendritic cell functions following trauma-hemorrhage

doi:10.1152/ajpcell.00447.2008

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Am J Physiol Cell Physiol 296: C124-C130, 2009. First published November 5, 2008; doi:10.1152/ajpcell.00447.2008
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RECEPTORS AND SIGNAL TRANSDUCTION

Effect of interleukin-15 on depressed splenic dendritic cell functions following trauma-hemorrhage

Takashi Kawasaki, Mashkoor A. Choudhry, Martin G. Schwacha, Kirby I. Bland, and Irshad H. Chaudry

Center for Surgical Research and Department of Surgery, University of Alabama at Birmingham, Birmingham, Alabama

Submitted 29 August 2008 ; accepted in final form 4 November 2008

Although trauma-hemorrhage (T-H) induces suppressed splenicdendritic cell (DC) maturation and antigen presentation capacity,it remains unclear whether IL-15 modulates splenic DC functions.The aim of this study therefore was to investigate the effectof IL-15 on splenic DC functions after T-H. Male C3H/HeN mice(6–8 wk old) were randomly assigned to T-H or sham operation.T-H was induced by midline laparotomy and $~$ 90 min of hemorrhagicshock (blood pressure 35 mmHg), followed by fluid resuscitation(4x the shed blood volume in the form of Ringer lactate). Twohours later, mice were killed, splenic DCs were isolated, andthe effects of exogenous IL-15 on their costimulatory factors,major histocompatibility class II expression, ability to producecytokines, and antigen presentation were measured. The resultsindicate that IL-15 production capacity of splenic DCs was reducedfollowing T-H. Ex vivo exposure to IL-15 attenuated the suppressedproduction of TNF- ${alpha}$ , IL-6, and IFN- ${gamma}$ from splenic DCs followingT-H. In addition, expression of surface antigen studies demonstratethat exogenous IL-15 attenuated T-H-induced downregulation ofthe activation of DC. The suppressed splenic DC antigen presentationfunction following T-H was also attenuated by IL-15 treatment.Moreover, IL-15 enhanced IL-12-induced IFN- ${gamma}$ production and antigenpresentation by splenic DCs. These data suggest that ex vivotreatment with IL-15 following T-H provides beneficial effectson splenic DCs. The depression in IL-15 production by splenicDCs could contribute to the host's enhanced susceptibility toinfections following T-H.

antigen presentation; tumor necrosis factor- ${alpha}$ ; major histocompatibility class II

Address for reprint requests and other correspondence: I. H. Chaudry, Center for Surgical Research, Univ. of Alabama at Birmingham, 1670 University Blvd., Volker Hall, Rm. G094, Birmingham, AL 35294-0019 (e-mail: irshad.chaudry{at}ccc.uab.edu)