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L-type calcium channel antagonism – Translation from in vitro to in vivo

离体 地尔硫卓 钙通道 体内 维拉帕米 药理学 电压依赖性钙通道 L型钙通道 硝苯地平 T型钙通道 二氢吡啶 化学 体外 医学 内科学 生物 生物化学 生物技术
作者
Bernard Fermini,David S. Ramirez,H. Sunny Sun,Asser Bassyouni,Michelle Hemkens,Todd Wisialowski,Stephen Jenkinson
出处
期刊:Journal of Pharmacological and Toxicological Methods [Elsevier BV]
卷期号:84: 86-92 被引量:10
标识
DOI:10.1016/j.vascn.2016.11.002
摘要

Although therapeutically beneficial in the treatment of certain diseases, L-type calcium channel antagonism can result in unwanted off-target pharmacology leading to adverse drug reactions and to the termination of the development of otherwise promising compounds. In the present study three marketed calcium channel inhibitors, nifedipine, verapamil and diltiazem were profiled in a series of in vitro and ex-vivo assays in an effort to determine the ability of these assays to discriminate, between dihydropyridine versus non-dihydropyridine-like compounds, and how well they can predict the cardiovascular effects observed in a conscious telemetered rat model. Standard calcium channel antagonists were profiled in radioligand binding, patch clamp and calcium flux assays. In addition, cardiovascular endpoints related to calcium channel activity were also examined in ex vivo tissue bath preparations, including relaxation of pre-constricted rat aorta and the guinea pig Langendorff isolated heart model. The data generated were correlated with in vivo blood pressure and heart rate data from conscious telemetered rats. Our results show that the binding, FLIPR and aorta assays allow differentiation of the compounds in two distinct classes of L-type calcium channel antagonists, and are good predictors of in vivo outcomes. These results suggest that in vitro and ex vivo profiling remains a valuable tool in predicting potential in vivo cardiovascular safety issues, and can aid in the selection of novel development compounds that show inherent inhibitory activity against L-type calcium channels.

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