Ischemic preconditioning prevents apoptotic cell death and necrosis in early and intermediate phases of liver ischemia-reperfusion injury in rats

Quireze Junior, Claudemiro [UNIFESP]; Montero, Edna Frasson de Souza [UNIFESP]; Leitao, Regina Maria Cubero [UNIFESP]; Juliano, Yara [UNIFESP]; Fagundes, Djalma José [UNIFESP]; Poli de Figueiredo, Luiz Francisco [UNIFESP]

Ischemic preconditioning prevents apoptotic cell death and necrosis in early and intermediate phases of liver ischemia-reperfusion injury in rats

Data

2006-07-01

Autores

Quireze Junior, Claudemiro [UNIFESP]

Montero, Edna Frasson de Souza [UNIFESP]

Leitao, Regina Maria Cubero [UNIFESP]

Juliano, Yara [UNIFESP]

Fagundes, Djalma José [UNIFESP]

Poli de Figueiredo, Luiz Francisco [UNIFESP]

Tipo

Artigo

Resumo

Ischemic preconditioning (IPC) may be useful in attenuating the hepatic ischemia reperfusion (IR) syndrome by means of improving cell resistance to anoxia and reoxygenation and preventing cell death. Since there are insufficient data available regarding the chronology of preconditioning effects, we investigated the role of IPC, to test the hypothesis that liver protection would occur during the early and intermediate phases of the reperfusion period. Wistar rats ( n = 72) were randomly assigned into six experimental groups, 12 animals each. A 40-min ischemia to the left lateral and median liver lobes was induced by selective hepatic pedicle clamping followed by 30 min or 240 min of reperfusion (IR30 and IR240). IPC groups (IPC30 and IPC240) underwent a 10 min of ischemia followed by 10 min of reperfusion preceding the definitive 40-min ischemic period. Sham-operated animals were followed for 30 and 240 min. Hepatic enzymes and histological evaluation were performed after the reperfusion period. Hepatic ischemia-reperfusion (IR30 and IR240) induced marked increases in liver enzymes levels after 30 min and particularly after 240 min. IPC effectively attenuated those enzymatic increases. Microvesicular steatosis was observed after 30 min, but not 240 min, of reperfusion in both IPC and IR livers. Necrosis was detected in 66.7% of IR240 and only in 8.3% of IPC240. Both hepatocyte and sinusoidal apoptosis were markedly attenuated by IPC. We conclude that IPC provided protection against hepatic ischemia reperfusion injury in early and intermediate phases of the reperfusion period, reducing hepatic enzymatic leakage and ameliorating hepatic apoptosis and necrosis.

Citação

Journal of Investigative Surgery. Philadelphia: Taylor & Francis Inc, v. 19, n. 4, p. 229-236, 2006.