A computer program for motion analysis of single cardiac myocytes.

U T Rüegg, J F Zuber, R Best
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引用次数: 3

Abstract

Single adult cardiac ventricular cells were prepared by collagenase perfusion of a rat heart. They were stimulated electrically in a perfusion chamber and their length changes were followed under a microscope. The motion was followed via a video camera and by a TV-line counting device and was recorded on-line by a personal computer. The program RECORD was used to calculate peak amplitude, base line drift and peak width at different peak heights allowing the determination of a number of variables of the cellular motion. The method was applied to drugs affecting the amplitude of contractions and the speed of relaxation. Results of beta-adrenergic stimulation, muscarinic inhibition and of the Ca(2+)-ATPase inhibitor cyclopiazonic acid (CPA) are shown. Besides its stimulatory effect on length, the beta-adrenergic agonist isoprenaline concentration-dependently shortened relaxation time. Carbachol reversed the increase in cellular shortening caused by isoprenaline in a concentration-dependent manner without fully reversing the shortened relaxation. CPA prolonged the return to diastole, presumably due to its inhibition of Ca(2+)-reuptake into the sarcoplasmatic reticulum.
用于单个心肌细胞运动分析的计算机程序。
采用胶原酶灌注法制备大鼠心肌单个心室细胞。在灌注室中电刺激它们,在显微镜下观察它们的长度变化。这一动作通过摄像机和电视线路计数装置进行跟踪,并由个人电脑在线记录下来。RECORD程序用于计算峰值振幅,基线漂移和不同峰高的峰宽,从而确定细胞运动的许多变量。该方法应用于影响收缩幅度和放松速度的药物。结果显示-肾上腺素能刺激,毒蕈碱抑制和Ca(2+)- atp酶抑制剂环吡唑酸(CPA)。肾上腺素能激动剂异丙肾上腺素除了对长度有刺激作用外,还能以浓度依赖性缩短松弛时间。Carbachol以浓度依赖的方式逆转了异丙肾上腺素引起的细胞缩短的增加,但没有完全逆转缩短的松弛。CPA延长了舒张期的恢复,可能是由于其抑制Ca(2+)-再摄取到肌浆网。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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