Kågström Jens, Sjögren Eva-Lena, Ericson Ann-Christin
Safety Pharmacology, Safety Assessment Sweden, AstraZeneca R&D Södertälje, S-151 85 Södertälje, Sweden.
J Pharmacol Toxicol Methods. 2007 Sep-Oct;56(2):186-93. doi: 10.1016/j.vascn.2007.03.003. Epub 2007 May 24.
While the dog in vivo model is commonly employed in the later phase of discovery for assessing drug-induced QT prolongation, an early screening assay is valuable when selecting compounds for further development and when compound availability usually is low. One such screening assay is the anaesthetised guinea pig monophasic action potential (MAP) model. The aim of the present study was to evaluate the ability of this model to detect proarrhythmic properties by testing a set of reference compounds with known clinical profile. Moreover, these results were compared to data previously obtained using in vivo canine QT assays (QT PRODACT study).
Anaesthetised and ventilated male guinea pigs were vagotomised and pretreated with propranolol. After thoracotomy, a pacing electrode was clipped to the left atrial appendage and a suction MAP electrode positioned on the left ventricular epicardium. The drug or corresponding vehicle was injected intravenously in cumulative doses and MAP duration at 90% repolarisation (MAPD90) was recorded during cardiac pacing.
The 8 drugs known to be proarrhythmic in the clinic all displayed dose-dependent prolongation of MAPD90, while the 4 drugs devoid of dysrhythmia in man had no effect. When comparing doses producing a 10% MAPD90 increase with doses reported to increase QTc by 10% in dogs a strong correlation was seen (R(2) 0.94 and 0.58 for anaesthetised and conscious dogs, respectively).
The guinea pig MAP assay identified all clinically positive drugs while negative drugs were without effect on ventricular repolarisation. Furthermore, a good concurrence is shown between the guinea pig and dog models in identifying compounds with proarrhythmic properties. Overall, the study reinforces the anaesthetised guinea pig MAP model as a reliable assay predicting QT liability of new chemical entities and as a highly sensitive early screening model for cardiovascular risk.
虽然犬体内模型通常用于药物研发后期评估药物诱导的QT间期延长,但在选择化合物进行进一步开发且化合物数量通常较少时,早期筛选试验很有价值。一种这样的筛选试验是麻醉豚鼠单相动作电位(MAP)模型。本研究的目的是通过测试一组具有已知临床特征的参考化合物,评估该模型检测致心律失常特性的能力。此外,将这些结果与先前使用体内犬QT试验(QT PRODACT研究)获得的数据进行比较。
对麻醉并通气的雄性豚鼠进行迷走神经切断术,并用普萘洛尔预处理。开胸后,将起搏电极夹在左心耳上,将吸引式MAP电极置于左心室心外膜上。以累积剂量静脉注射药物或相应的赋形剂,并在心脏起搏期间记录90%复极化时的MAP持续时间(MAPD90)。
临床上已知有致心律失常作用的8种药物均显示MAPD90呈剂量依赖性延长,而在人体中无心律失常作用的4种药物则无影响。当将使MAPD90增加10%的剂量与据报道使犬QTc增加10%的剂量进行比较时,发现有很强的相关性(麻醉犬和清醒犬的R(2)分别为0.94和0.58)。
豚鼠MAP试验识别出所有临床上呈阳性的药物,而阴性药物对心室复极化无影响。此外,在识别具有致心律失常特性的化合物方面,豚鼠模型和犬模型之间显示出良好的一致性。总体而言,该研究强化了麻醉豚鼠MAP模型作为预测新化学实体QT风险的可靠试验以及作为心血管风险高度敏感的早期筛选模型的地位。
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