Effect of Peroxisome Proliferator-Activated Receptor Alpha Activators on Tumor Necrosis Factor Expression in Mice during Endotoxemia

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Infection and Immunity, July 1999, p. 3488-3493, Vol. 67, No. 7
0019-9567/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.

Effect of Peroxisome Proliferator-Activated Receptor Alpha Activators on Tumor Necrosis Factor Expression in Mice during Endotoxemia

Molly R. Hill,¹^,²^,^* Stephen Clarke,³ Kerry Rodgers,² Brandi Thornhill,² Jeffrey M. Peters,⁴ Frank J. Gonzalez,⁴ and Jeffrey M. Gimble⁵^,⁶^,⁷

Departments of Radiologic Technology,¹ Surgery,⁵ and Pathology,⁶ University of Oklahoma Health Sciences Center, Oklahoma City, Oklahoma 73190; Department of Zoology, University of Oklahoma, Norman, Oklahoma 73019⁷; Department of Biological Sciences, Oklahoma Christian University, Oklahoma City, Oklahoma 73136²; Laboratory of Metabolism, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892⁴; and Department of Nutritional Science, University of Wisconsin, Madison, Wisconsin 53706³

Received 30 October 1998/Returned for modification 29 December 1998/Accepted 21 April 1999

Inflammatory mediators orchestrate the host immune and metabolic response to acute bacterial infections and mediate the eventsleading to septic shock. Tumor necrosis factor (TNF) has longbeen identified as one of the proximal mediators of endotoxinaction. Recent studies have implicated peroxisome proliferator-activatedreceptor alpha (PPAR $alpha$ ) as a potential target to modulate regulationof the immune response. Since PPAR $alpha$ activators, which are hypolipidemicdrugs, are being prescribed for a significant population of olderpatients, it is important to determine the impact of these drugson the host response to acute inflammation. Therefore, we examinedthe role of PPAR $alpha$ activators on the regulation of TNF expressionin a mouse model of endotoxemia. CD-1 mice treated with dietaryfenofibrate or Wy-14,643 had fivefold-higher lipopolysaccharide(LPS)-induced TNF plasma levels than LPS-treated control-fed animals.Higher LPS-induced TNF levels in drug-fed animals were reflectedphysiologically in significantly lower glucose levels in plasmaand a significantly lower 50% lethal dose than those in LPS-treatedcontrol-fed animals. Utilizing PPAR $alpha$ wild-type (WT) and knockout(KO) mice, we showed that the effect of fenofibrate on LPS-inducedTNF expression was indeed mediated by PPAR $alpha$ . PPAR $alpha$ WT mice fedfenofibrate also had a fivefold increase in LPS-induced TNF levelsin plasma compared to control-fed animals. However, LPS-inducedTNF levels were significantly decreased and glucose levels inplasma were significantly increased in PPAR $alpha$ KO mice fed fenofibratecompared to those in control-fed animals. Data from peritonealmacrophage studies indicate that Wy-14,643 modestly decreasedTNF expression in vitro. Similarly, overexpression of PPAR $alpha$ in293T cells decreased activity of a human TNF promoter-luciferaseconstruct. The results from these studies suggest that any anti-inflammatoryactivity of PPAR $alpha$ in vivo can be masked by other systemic effectsof PPAR $alpha$ activators.

^* Corresponding author. Mailing address: Department of Radiologic Technology, OUHSC, P.O. Box 26901, Oklahoma City, OK 73190.Phone: (405) 425-5459. Fax: (405) 425-5446. E-mail: Molly.Hill{at}oc.edu.

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