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KMID : 0620920150470060002
Experimental & Molecular Medicine
2015 Volume.47 No. 6 p.2 ~ p.2
Effects of sevoflurane on tight junction protein expression and PKC-¥á translocation after pulmonary ischemia?reperfusion injury
Jun Chai

Bo Long
Xiaomei Liu
Yan Li
Ning Han
Ping Zhao
Weimin Chen
Abstract
Pulmonary dysfunction caused by ischemia-reperfusion injury is the leading cause of mortality in lung transplantation. We aimed to investigate the effects of sevoflurane pretreatment on lung permeability, tight junction protein occludin and zona occludens 1 (ZO-1) expression, and translocation of protein kinase C (PKC)-¥á after ischemia?reperfusion. A lung ischemia-reperfusion injury model was established in 96 male Wistar rats following the modified Eppinger method. The rats were divided into four groups with 24 rats in each group: a control (group C), an ischemia-reperfusion group (IR group), a sevoflurane control group (sev-C group), and a sevoflurane ischemia-reperfusion group (sev?IR group). There were three time points in each group: ischemic occlusion for 45?min, reperfusion for 60?min and reperfusion for 120?min; and there were six rats per time point. For the 120-min reperfusion group, six extra rats underwent bronchoalveolar lavage. Mean arterial pressure (MAP) and pulse oxygen saturation (SpO2) were recorded at each time point. The wet/dry weight ratio and lung permeability index (LPI) were measured. Quantitative RT-PCR and Western blot were used to measure pulmonary occludin and ZO-1, and Western blot was used to measure cytosolic and membranous PKC-¥á in the lung. Lung permeability was significantly increased after ischemia?reperfusion. Sevoflurane pretreatment promoted pulmonary expression of occludin and ZO-1 after reperfusion and inhibited the translocation of PKC-¥á. In conclusion, sevoflurane pretreatment alleviated lung permeability by upregulating occludin and ZO-1 after ischemia?reperfusion. Sevoflurane pretreatment inhibited the translocation and activation of PKC-¥á, which also contributed to the lung-protective effect of sevoflurane.
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