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使用电场聚焦和阻抗的安全药理学研究。

Safety pharmacology studies using EFP and impedance.

作者信息

Obergrussberger Alison, Juhasz Krisztina, Thomas Ulrich, Stölzle-Feix Sonja, Becker Nadine, Dörr Leo, Beckler Matthias, Bot Corina, George Michael, Fertig Niels

机构信息

Nanion Technologies GmbH, Gabrielenstr. 9, 80636 Munich, Germany.

Nanion Technologies GmbH, Gabrielenstr. 9, 80636 Munich, Germany.

出版信息

J Pharmacol Toxicol Methods. 2016 Sep-Oct;81:223-32. doi: 10.1016/j.vascn.2016.04.006. Epub 2016 Apr 12.

Abstract

INTRODUCTION

While extracellular field potential (EFP) recordings using multi-electrode arrays (MEAs) are a well-established technique for monitoring changes in cardiac and neuronal function, impedance is a relatively unexploited technology. The combination of EFP, impedance and human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) has important implications for safety pharmacology as functional information about contraction and field potentials can be gleaned from human cardiomyocytes in a beating monolayer. The main objectives of this study were to demonstrate, using a range of different compounds, that drug effects on contraction and electrophysiology can be detected using a beating monolayer of hiPSC-CMs on the CardioExcyte 96.

METHODS

hiPSC-CMs were grown as a monolayer on NSP-96 plates for the CardioExcyte 96 (Nanion Technologies) and recordings were made in combined EFP and impedance mode at physiological temperature. The effect of the hERG blockers, E4031 and dofetilide, hERG trafficking inhibitor, pentamidine, β-adrenergic receptor agonist, isoproterenol, and calcium channel blocker, nifedipine, was tested on the EFP and impedance signals.

RESULTS

Combined impedance and EFP measurements were made from hiPSC-CMs using the CardioExcyte 96 (Nanion Technologies). E4031 and dofetilide, known to cause arrhythmia and Torsades de Pointes (TdP) in humans, decreased beat rate in impedance and EFP modes. Early afterdepolarization (EAD)-like events, an in vitro marker of TdP, could also be detected using this system. Isoproterenol and nifedipine caused an increase in beat rate. A long-term study (over 30h) of pentamidine, a hERG trafficking inhibitor, showed a concentration and time-dependent effect of pentamidine.

DISCUSSION

In the light of the new Comprehensive in Vitro Proarrhythmia Assay (CiPA) initiative to improve guidelines and standardize assays and protocols, the use of EFP and impedance measurements from hiPSCs may become critical in determining the proarrhythmic risk of potential drug candidates. The combination of EFP offering information about cardiac electrophysiology, and impedance, providing information about contractility from the same area of a synchronously beating monolayer of human cardiomyocytes in a 96-well plate format has important implications for future cardiac safety testing.

摘要

引言

虽然使用多电极阵列(MEA)进行细胞外场电位(EFP)记录是监测心脏和神经功能变化的一项成熟技术,但阻抗技术相对未得到充分利用。EFP、阻抗与人类诱导多能干细胞衍生的心肌细胞(hiPSC-CMs)相结合,对于安全药理学具有重要意义,因为可以从跳动的单层人类心肌细胞中获取有关收缩和场电位的功能信息。本研究的主要目的是使用一系列不同的化合物,证明在CardioExcyte 96上使用hiPSC-CMs的跳动单层可以检测药物对收缩和电生理的影响。

方法

将hiPSC-CMs作为单层培养在用于CardioExcyte 96(Nanion Technologies)的NSP-96板上,并在生理温度下以EFP和阻抗组合模式进行记录。测试了hERG阻滞剂E4031和多非利特、hERG转运抑制剂喷他脒、β-肾上腺素能受体激动剂异丙肾上腺素和钙通道阻滞剂硝苯地平对EFP和阻抗信号的影响。

结果

使用CardioExcyte 96(Nanion Technologies)对hiPSC-CMs进行了阻抗和EFP联合测量。已知会在人类中引起心律失常和尖端扭转型室速(TdP)的E4031和多非利特,在阻抗和EFP模式下降低了搏动率。使用该系统还可以检测到早期后去极化(EAD)样事件,这是TdP的一种体外标志物。异丙肾上腺素和硝苯地平导致搏动率增加。对hERG转运抑制剂喷他脒进行的一项长期研究(超过30小时)显示了喷他脒的浓度和时间依赖性效应。

讨论

鉴于新的体外全面致心律失常试验(CiPA)倡议旨在改进指南并规范试验和方案,使用来自hiPSC的EFP和阻抗测量可能在确定潜在药物候选物的致心律失常风险方面变得至关重要。EFP提供有关心脏电生理的信息,而阻抗则从96孔板格式的同步跳动单层人类心肌细胞的同一区域提供有关收缩性的信息,这种组合对未来的心脏安全性测试具有重要意义。

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