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己酮可可碱对肺移植后再灌注损伤的改善作用。巴黎南大学肺移植研究小组。

Amelioration of reperfusion injury by pentoxifylline after lung transplantation. The Université Paris-Sud Lung Transplant Group.

作者信息

Chapelier A, Reignier J, Mazmanian M, Dulmet E, Libert J M, Dartevelle P, Barbotin F, Hervé P

机构信息

Laboratoire de Chirurgie Expérimentale, Hôpital Marie Lannelongue, Université Paris Sud, Le Plessis Robinson, France.

出版信息

J Heart Lung Transplant. 1995 Jul-Aug;14(4):676-83.

PMID:7578175
Abstract

BACKGROUND

Pentoxifylline attenuates neutrophil-mediated lung injury in several models of acute lung inflammation.

METHODS

Because pulmonary neutrophil sequestration is the main determinant of lung reperfusion injury, we sought to determine whether pentoxifylline prevented reperfusion injury in isolated perfused rat lung (4-hour cold ischemia, 1-hour reperfusion; pentoxifylline intravenously 40 mg) and in pigs after left lung allotransplantation (24-hour cold ischemia, 4-hour reperfusion; pentoxifylline 1.5 mg/kg/hr intravenously). In the pigs, inflatable cuffs placed around each pulmonary artery enabled us to evaluate each lung separately.

RESULTS

In rat lungs, the coefficient of lung permeability increased by 75% +/- 10% in controls and by 3% +/- 2% (p < 0.01) in pentoxifylline-treated lungs. In the pigs, with blood flow to the transplanted lung alone and ventilation with an inspired oxygen fraction of 1, the arterial oxygen tension was greater in the pentoxifylline group than in the control group (423 +/- 49 versus 265 +/- 43 mm Hg, p < 0.05), whereas the total pulmonary vascular resistance was lower (15 +/- 1 versus 30 +/- 9 mm Hg/L/min, p < 0.02). After reperfusion, the decrease in circulating leukocyte count fell by 35% +/- 3% in the control group and remained unchanged in the pentoxifylline group, and the leukocytes count per microscopic field in the transplanted lung was lower in the pentoxifylline group than in the control group (15 +/- 2 versus 140 +/- 50, p < 0.02).

CONCLUSIONS

These data suggest that pentoxifylline prevented reperfusion injury by decreasing neutrophil lung sequestration.

摘要

背景

己酮可可碱在多种急性肺部炎症模型中可减轻中性粒细胞介导的肺损伤。

方法

由于肺中性粒细胞滞留是肺再灌注损伤的主要决定因素,我们试图确定己酮可可碱是否能预防离体灌注大鼠肺(4小时冷缺血,1小时再灌注;静脉注射己酮可可碱40毫克)以及左肺同种异体移植猪(24小时冷缺血,4小时再灌注;静脉注射己酮可可碱1.5毫克/千克/小时)的再灌注损伤。在猪身上,围绕每条肺动脉放置的可充气袖带使我们能够分别评估每侧肺。

结果

在大鼠肺中,对照组肺通透性系数增加了75%±10%,而己酮可可碱治疗组增加了3%±2%(p<0.01)。在猪身上,仅对移植肺供血并给予吸入氧分数为1的通气时,己酮可可碱组的动脉血氧张力高于对照组(423±49对265±43毫米汞柱,p<0.05),而总肺血管阻力较低(15±1对30±9毫米汞柱/升/分钟,p<0.02)。再灌注后,对照组循环白细胞计数下降了35%±3%,而己酮可可碱组保持不变,且己酮可可碱组移植肺每高倍视野白细胞计数低于对照组(15±2对140±50,p<0.02)。

结论

这些数据表明,己酮可可碱通过减少中性粒细胞在肺中的滞留预防了再灌注损伤。

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