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Pentoxifylline Reduces Leukocyte Retention in the Coronary Microcirculation Early in Reperfusion following Ischemia

 

作者: Leslie S. Ritter,   D.S. Wilson,   S.K. Williams,   J.G. Copeland,   P.F. McDonagh,  

 

期刊: International Journal of Microcirculation  (Karger Available online 1996)
卷期: Volume 16, issue 4  

页码: 170-179

 

ISSN:0167-6865

 

年代: 1996

 

DOI:10.1159/000179170

 

出版商: S. Karger AG

 

关键词: Coronary microcirculation;Ischemia-reperfusion;Leukocytes;Pentoxifylline;Rat;Reperfusion injury

 

数据来源: Karger

 

摘要:

Using direct visualization techniques, we recently confirmed earlier histologic studies that leukocytes accumulate primarily in the coronary capillaries of ischemic hearts during early reperfusion. The purpose of this study was to determine if pentoxifylline (PTX) would reduce leukocyte trapping in postischemic hearts. Isolated rat hearts were subjected to 30 min of 37 °C, no-flow ischemia. Hearts were initially reperfused with diluted whole blood containing fluorescent leukocytes. At 5, (R5), 20, and 35 min of reperfusion, the deposition of leukocytes in the coronary capillaries and venules was observed directly using intravital fluorescence microscopy. Three groups were studied: a non-ischemic control group (group I) and postischemic groups reperfused with diluted whole blood treated with vehicle group II or PTX (5 mM; group III). Postischemic reperfusion with unactivated blood caused a significant trapping of leukocytes in coronary capillaries throughout reperfusion (R5, group I = 2.0 ± 0.3 vs. group II = 5.7 ± 0.6 leukocytes/capillary field, p < 0.05). The addition of PTX reduced capillary leukocyte trapping below control values throughout reperfusion (R5, group III = 1.6 ± 0.2 leukocytes/capillary field, p < 0.05). At R5, there was no statistically significant difference in leukocyte accumulation in venules for all groups (group I = 1.5 ± 0.6, group II = 3.2 ± 0.4, group III = 3.3 ± 0.4 leukocytes/100 µm venule). During the reperfusion period, leukocyte persistence in the capillaries of postischemic hearts (36%) was greater than in the venules (13%). These data indicate that early in reperfusion after myocardial ischemia, leukocyte trapping occurs primarily in the coronary capillaries. PTX reduced early leukocyte trapping in the capillaries. The results also demonstrate that during reperfusion, the mechanisms affecting capillary retention are more persistent than those in the venule. These findings suggest that attempts to attenuate the damaging potential of early leukostasis in capillaries consider the biophysical properties of the le

 

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