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Department of Surgery, Temple University School of Medicine, Philadelphia, Pennsylvania 19140; Department of Surgery, University of Texas at Dallas Southwestern Medical Center, Dallas 75235; and Dallas Department of Veterans Affairs Medical Center, Dallas, Texas 75216
Received 6 April 1995; accepted in final form 15 May 1997.
Rothenbach, Patricia, Richard H. Turnage, Jose Iglesias,
Angela Riva, Lori Bartula, and Stuart I. Myers. Downstream effects
of splanchnic ischemia-reperfusion injury on renal function and
eicosanoid release. J. Appl. Physiol.
82(2): 530-536, 1997.
This study examines the hypothesis that
intestinal ischemia-reperfusion (I/R) injury contributes to renal
dysfunction by altered renal eicosanoid release. Anesthetized
Sprague-Dawley rats underwent 60 min of sham or superior mesenteric
artery (SMA) occlusion with 60 min of reperfusion. The I/R groups
received either allopurinol, pentoxifylline, 1-benzylimidazole, or
carrier before SMA occlusion. In vivo renal artery blood flow was
measured by Transonic flow probes, the kidneys were then perfused in
vitro for 30 min, and the effluent was analyzed for eicosanoid release
and renal function. Intestinal I/R caused a twofold increase in the
ratio of renal release of thromboxane
B2 to prostaglandin
E2 and to 6-ketoprostaglandin F1
compared with the sham
level, with a corresponding 25% decrease in renal sodium and inulin
clearance and renal blood flow. Pentoxifylline or allopurinol
pretreatment restored renal eicosanoid release and renal sodium and
inulin clearance to the sham level but did not alter renal blood flow.
Pretreatment with 1-benzylimidazole restored renal function, eicosanoid
release, and renal blood flow to sham levels. These data suggest that
severe intestinal I/R contributes to the downregulation of renal
function. The decrease in renal function is due in part to toxic oxygen metabolites, which occur in the milieu of altered renal eicosanoid release, reflecting a decrease in vasodilator and an increase in
vasoconstrictor eicosanoids.
renal eicosanoid release; renal blood flow
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