用于评估蒽环类药物心脏毒性及其规避方法的大鼠离体灌注心脏模型的建立。
Development of the model of rat isolated perfused heart for the evaluation of anthracycline cardiotoxicity and its circumvention.
作者信息
Pouna P, Bonoron-Adèle S, Gouverneur G, Tariosse L, Besse P, Robert J
机构信息
Department of Medical Biochemistry and Molecular Biology, University of Bordeaux II, France.
出版信息
Br J Pharmacol. 1996 Apr;117(7):1593-9. doi: 10.1111/j.1476-5381.1996.tb15326.x.
Abstract
- In order to develop a predictive model for the preclinical evaluation of anthracycline cardiotoxicity and the means of preventing it, we have studied the functional parameters of perfused hearts isolated from rats receiving repeated doses of several anthracyclines. 2. The anthracyclines studied were doxorubicin, epirubicin, pirarubicin and daunorubicin, and we also studied a liposomal formulation of daunorubicin (DaunoXome) and the co-administration of dexrazoxane (ICRF-187) and doxorubicin. 3. Anthracyclines were administered i.p. at equimolar doses corresponding to 3 mg kg-1 per injection of doxorubicin, every other day for a total of six doses. Dexrazoxane was used at the dose of 30 mg kg-1 per injection and was administered either 30 min before or 30 min after doxorubicin. We evaluated any general toxicity towards the animals as well as alterations of left ventricular contractility and relaxation ex vivo. 4. Epirubicin and daunorubicin were significantly less cardiotoxic than doxorubicin, and neither pirarubicin nor DaunoXome caused significant alterations in cardiac function. There was a direct relationship between the decrease in cardiac contractility or relaxation and anthracycline accumulation in the heart, evaluated after the same treatment schedule. 5. Dexrazoxane induced a significant protection against doxorubicin-induced cardiac toxicity when administered 30 min before doxorubicin, whereas this protection was ineffective when administered 30 min after doxorubicin. Direct perfusion of DaunoXome in isolated hearts of untreated animals resulted in a 12-fold reduction of the accumulation of daunorubicin in heart tissue as compared to the perfusion of free daunorubicin, and did not cause alterations in cardiac function at a dosage for which free daunorubicin induced major alterations. 6. The isolated perfused rat heart appears to be a valuable model for screening of new anthracyclines and of strategies for circumventing anthracycline cardiotoxicity.
摘要
- 为了开发一种用于蒽环类药物心脏毒性临床前评估及其预防方法的预测模型,我们研究了从接受多次不同蒽环类药物剂量的大鼠分离出的灌注心脏的功能参数。2. 所研究的蒽环类药物有阿霉素、表阿霉素、吡柔比星和柔红霉素,我们还研究了柔红霉素的脂质体制剂(DaunoXome)以及右丙亚胺(ICRF - 187)与阿霉素的联合给药。3. 蒽环类药物以等摩尔剂量腹腔注射,相当于每次注射阿霉素3 mg kg⁻¹,每隔一天注射一次,共注射六次。右丙亚胺的使用剂量为每次注射30 mg kg⁻¹,在阿霉素注射前30分钟或注射后30分钟给药。我们评估了对动物的任何一般毒性以及离体左心室收缩性和舒张性的改变。4. 表阿霉素和柔红霉素的心脏毒性明显低于阿霉素,吡柔比星和DaunoXome均未引起心脏功能的显著改变。在相同治疗方案后评估,心脏收缩性或舒张性的降低与心脏中蒽环类药物的蓄积之间存在直接关系。5. 右丙亚胺在阿霉素注射前30分钟给药时,对阿霉素诱导的心脏毒性有显著保护作用,而在阿霉素注射后30分钟给药时,这种保护作用无效。在未治疗动物的离体心脏中直接灌注DaunoXome,与灌注游离柔红霉素相比,心脏组织中柔红霉素的蓄积减少了12倍,并且在游离柔红霉素诱导主要改变的剂量下,未引起心脏功能的改变。6. 离体灌注大鼠心脏似乎是筛选新蒽环类药物和规避蒽环类药物心脏毒性策略的有价值模型。
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