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肝动脉内输注5-氟尿嘧啶(5-FU)后的心肺血流动力学和药代动力学。猪的实验研究。

Cardiopulmonary hemodynamics and pharmacokinetics after hepatic intraarterial infusion of 5-fluorouracil (5-FU). An experimental study in the pig.

作者信息

Andersson M, Domellöf L, Häggmark S, Johansson G, Reiz S, Gustavsson B

机构信息

Department of Surgery, University Hospital, Umeå, Sweden.

出版信息

Cancer Chemother Pharmacol. 1988;22(3):251-5. doi: 10.1007/BF00273420.

Abstract

Reported 5-FU-induced cardiac side effects may be explained by drug-induced hemodynamic changes and/or by direct myocardial toxicity due to regional drug uptake. This question was studied in 11 animals given constant infusions and 6 animals given bolus 5-FU infusions into the hepatic artery. Six animals, which received normal saline infusion, served as controls. A second aim was to study possible pulmonary drug clearance. Aortic, pulmonary arterial, and coronary sinus plasma 5-FU concentrations were determined during constant and after the bolus infusions of 5-FU. The V5 ECG, aortic, pulmonary arterial, and right atrial pressures were recorded continuously, and cardiac output and coronary sinus blood flow were recorded intermittently in all animals. No significant alterations in hemodynamic variables were seen during constant infusion. After the bolus infusion, an increased arterio-mixed venous oxygen content difference was recorded. Pharmacokinetic data after 3-min infusions indicated pulmonary drug uptake and release; during constant infusions, the data indicated myocardial drug uptake. As there were no alterations in myocardial oxygen demand or supply or in systemic hemodynamics during this myocardial drug uptake, it is likely that the cardiotoxicity is related to the direct effects of the drug on cardiac myocytes.

摘要

报道的5-氟尿嘧啶(5-FU)引起的心脏副作用可能是由药物诱导的血流动力学变化和/或由于局部药物摄取导致的直接心肌毒性所解释。在11只接受持续输注的动物和6只接受肝动脉大剂量5-FU输注的动物中研究了这个问题。6只接受生理盐水输注的动物作为对照。第二个目的是研究可能的肺部药物清除情况。在5-FU持续输注期间和大剂量输注后,测定主动脉、肺动脉和冠状窦血浆中5-FU的浓度。在所有动物中连续记录V5心电图、主动脉、肺动脉和右心房压力,并间歇记录心输出量和冠状窦血流量。在持续输注期间,血流动力学变量未见明显改变。大剂量输注后,记录到动-混合静脉氧含量差增加。3分钟输注后的药代动力学数据表明肺部有药物摄取和释放;在持续输注期间,数据表明心肌有药物摄取。由于在这种心肌药物摄取过程中心肌氧需求或供应以及全身血流动力学均无改变,因此心脏毒性可能与药物对心肌细胞的直接作用有关。

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