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体外循环期间心脏前列环素的动力学

Cardiac prostacyclin kinetics during cardiopulmonary bypass.

作者信息

Kobinia G S, LaRaia P J, Peterson M B, D'Ambra M N, Watkins W D, Austen W G, Buckley M J

出版信息

J Thorac Cardiovasc Surg. 1984 Dec;88(6):965-71.

PMID:6389992
Abstract

We have investigated the response of systemic and myocardial prostacyclin metabolism to cardiopulmonary bypass and 30 minutes of hypothermic (22 degrees C), hyperkalemic (25 mEq K+) surgical cardioplegia. Thirteen adult mongrel dogs of either sex (range 21 to 36 kg) underwent sterile cardiopulmonary bypass without donor blood. Prostacyclin levels were obtained after cannulation, 20 minutes after onset of partial bypass, and 5 seconds after the onset of cardioplegia 1 (CP-1) and cardioplegia 2 (CP-2, 30 minutes later). Samples were drawn from the thoracic aorta, the aortic root below cross-clamping, and the coronary sinus. The stable metabolite of prostacyclin, 6-keto-PGF1 alpha was measured by double-antibody radioimmunoassay (pg/ml; values +/- standard error of the mean). We found that the onset of partial bypass is associated with significant increase in the systemic production of 6-keto-PGF1 alpha (122 +/- 33 versus 518 +/- 187; p less than 0.05), which persists throughout the experiment. A small but significant positive cardiac gradient of 6-keto-PGF1 alpha is found after cannulation (aortic root 122 +/- 33, coronary sinus 202 +/- 57, p less than 0.05). This gradient is more pronounced during partial bypass (aortic root 518 +/- 187, coronary sinus 686 +/- 186 p less than 0.05), when significant cardiac lactate extraction (p less than 0.005) is observed. After cross-clamping, a significantly increased gradient of 6-keto-PGF1 alpha is found during CP-1 (aortic root 74 +/- 10, coronary sinus 264 +/- 46, p less than 0.05 versus cannulation) in the presence of significant cardiac lactate production (p less than 0.005). A further significant increase in 6-keto-PGF1 alpha production is noted during the CP-2 infusion (aortic root 73 +/- 10, coronary sinus 483 +/- 83; p less than 0.01 versus CP-1), which is inversely related to cardiac oxygen uptake and endocardial/epicardial flow ratio. Our data demonstrate significant production of prostacyclin in the systemic and cardiac circulations during cardiopulmonary bypass and surgical cardioplegia. They further indicate that both ischemic and nonischemic stimuli regulate prostacyclin metabolism during cardiopulmonary bypass.

摘要

我们研究了全身和心肌前列环素代谢对体外循环及30分钟低温(22摄氏度)、高钾(25毫当量钾)心脏停搏液灌注的反应。13只成年杂种犬(雌雄不限,体重21至36千克)在无供血的情况下接受了无菌体外循环。在插管后、部分体外循环开始20分钟后、心脏停搏液1(CP - 1)开始5秒后以及30分钟后的心脏停搏液2(CP - 2)开始5秒后获取前列环素水平。样本取自胸主动脉、交叉钳夹下方的主动脉根部以及冠状窦。通过双抗体放射免疫测定法(皮克/毫升;数值±均值标准误差)测量前列环素的稳定代谢产物6 - 酮 - PGF1α。我们发现部分体外循环开始与全身6 - 酮 - PGF1α生成显著增加相关(122±33对518±187;p<0.05),且在整个实验过程中持续存在。插管后发现6 - 酮 - PGF1α存在微小但显著的正向心脏梯度(主动脉根部122±33,冠状窦202±57,p<0.05)。在部分体外循环期间该梯度更为明显(主动脉根部518±187,冠状窦686±186,p<0.05),此时观察到显著的心肌乳酸摄取(p<0.005)。交叉钳夹后,在CP - 1期间6 - 酮 - PGF1α梯度显著增加(主动脉根部74±10,冠状窦264±46,与插管相比p<0.05),同时存在显著的心肌乳酸生成(p<0.005)。在CP - 2灌注期间6 - 酮 - PGF1α生成进一步显著增加(主动脉根部73±10,冠状窦483±83;与CP - 1相比p<0.01),这与心肌氧摄取及心内膜/心外膜血流比值呈负相关。我们的数据表明在体外循环和心脏停搏液灌注期间全身和心脏循环中存在显著的前列环素生成。它们还进一步表明在体外循环期间缺血和非缺血刺激均调节前列环素代谢。

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