Ischemia–reperfusion rat model of acute pancreatitis: protein carbonyl as a putative early biomarker of pancreatic injury

Abstract

Acute pancreatitis (AP) is an inflammatory disorder that can affect adjacent and/or remote organs. Some evidence indicates that the production of reactive oxygen species is able to induce AP. Protein carbonyl (PC) derivatives, which can also be generated through oxidative cleavage mechanisms, have been implicated in several diseases, but there is little or no information on this bio marker in AP. We investigated the association between some inflammatory mediators and PC, with the severity of ischemia–reperfusion AP. Wistar rats (n = 56) were ran domly assigned in the following groups : control; sham, 15- or 180-min clamping of splenic artery, with 24 or 72 h of follow-up. The relationships between serum level of PC and thiobarbituric acid reactive species (TBARS) to mye loperoxidase (MPO) activity in tissue homogenates and to cytokines in culture supernatants of pancreatic samples were analyzed. MPO activity was related to the histology scores and increased in all clamping groups. Tumor necrosis factor-alpha (TNF-a), interleukin 1 beta (IL-1b), and interleukin-6 were higher in the 180-min groups. Sig nificant correlations were found between MPO activity and the concentrations of TNF-a and IL-1b. PC levels increased in the 15-min to 24-h group. TBARS levels were not altered substantially. MPO activity and TNF-a and IL 1b concentrations in pancreatic tissue are correlated with AP severity. Serum levels of PC appear to begin to rise early in the course of the ischemia–reperfusion AP and are no longer detected at later stages in the absence of severe pancreatitis. These data suggest that PC can be an efficient tool for the diagnosis of early stages of AP.