Inhibition of apoptosis induced by ischemia-reperfusion prevents inflammation
Marc A.R.C. Daemen, … , Peter Vandenabeele, Wim A. Buurman
Marc A.R.C. Daemen, … , Peter Vandenabeele, Wim A. Buurman
Published September 1, 1999
Citation Information: J Clin Invest. 1999;104(5):541-549. https://doi.org/10.1172/JCI6974.
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Article

Inhibition of apoptosis induced by ischemia-reperfusion prevents inflammation

Abstract

Ischemia followed by reperfusion leads to severe organ injury and dysfunction. Inflammation is considered to be the most important cause of tissue injury in organs subjected to ischemia. The mechanism that triggers inflammation and organ injury after ischemia remains to be elucidated, although different causes have been postulated. We investigated the role of apoptosis in the induction of inflammation and organ damage after renal ischemia. Using a murine model, we demonstrate a relationship between apoptosis and subsequent inflammation. At the time of reperfusion, administration of the antiapoptotic agents IGF-1 and ZVAD-fmk (a caspase inactivator) prevented the early onset of not only renal apoptosis, but also inflammation and tissue injury. Conversely, when the antiapoptotic agents were administered after onset of apoptosis, these protective effects were completely abrogated. The presence of apoptosis was directly correlated with posttranslational processing of the endothelial monocyte-activating polypeptide II (EMAP-II), which may explain apoptosis-induced influx and sequestration of leukocytes in the reperfused kidney. These results strongly suggest that apoptosis is a crucial event that can initiate reperfusion-induced inflammation and subsequent tissue injury. The newly described pathophysiological insights provide important opportunities to effectively prevent clinical manifestations of reperfusion injury in the kidney, and potentially in other organs.

Authors

Marc A.R.C. Daemen, Cornelis van ‘t Veer, Geertrui Denecker, Vincent H. Heemskerk, Tim G.A.M. Wolfs, Matthias Clauss, Peter Vandenabeele, Wim A. Buurman

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Figure 5

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Representative light micrographs (a and b) showing infiltrating neutroph...
Representative light micrographs (a and b) showing infiltrating neutrophils in areas with impaired renal morphological integrity in biopsies obtained from mice subjected to renal I/R after 1 day of reperfusion (a). Neutrophils were stained with the anti-murine neutrophil mAb Gr-1. Neither loss of morphological integrity nor infiltrating neutrophils were observed in kidneys obtained from sham-operated mice (b) (×200). Neutrophil influx was assessed quantitatively by determination of MPO increase at 2 hours and 1 day of reperfusion (c). Values are presented relative to the amount of MPO present in the contralateral kidney harvested immediately after reperfusion, and then normalized with respect to the MPO increase at day 1 in PBS-treated mice subjected to I/R. *P < 0.05 vs. control-treated animals. The data shown are mean ± SEM.