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Simultaneous optical mapping of transmembrane potential and wall motion in isolated perfused whole hearts

机译:隔离灌注的全心脏中跨膜电位和壁运动的同时光学映射

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摘要

Optical mapping of cardiac propagation has traditionally been hampered by motion artifact, chiefly due to changes in photodetector-to-tissue registration as the heart moves. We have developed an optical mapping technique to simultaneously record electrical waves and mechanical contraction in isolated hearts. This allows removal of motion artifact from transmembrane potential (Vm) recordings without the use of electromechanical uncoupling agents and allows the interplay of electrical and mechanical events to be studied at the whole organ level. Hearts are stained with the voltage-sensitive dye di-4-ANEPPS and ring-shaped markers are attached to the epicardium. Fluorescence, elicited on alternate frames by 450 and 505 nm light-emitting diodes, is recorded at 700 frames/ per second by a camera fitted with a 605±25 nm emission filter. Marker positions are tracked in software. A signal, consisting of the temporally interlaced 450 and 505 nm fluorescence, is collected from the pixels enclosed by each moving ring. After deinterlacing, the 505 nm signal consists of Vm with motion artifact, while the 450 nm signal is minimally voltage-sensitive and contains primarily artifacts. The ratio of the two signals estimates Vm. Deformation of the tissue enclosed by each set of 3 rings is quantified using homogeneous finite strain.
机译:传统上,运动传播伪影阻碍了心脏传播的光学映射,这主要是由于随着心脏移动,光电探测器到组织的配准发生了变化。我们已经开发了一种光学映射技术,可以同时记录离体心脏中的电波和机械收缩。这样可以在不使用机电解偶联剂的情况下从跨膜电位(Vm)记录中去除运动伪影,并可以在整个器官水平研究电气和机械事件的相互作用。心脏用电压敏感染料di-4-ANEPPS染色,并将环形标记物附着在心外膜上。装有605±25 nm发射滤光片的摄像机以450帧/秒的速度记录每秒450和505 nm发光二极管在交替帧上引发的荧光。标记位置在软件中跟踪。从每个移动环包围的像素中收集一个信号,该信号由时间上交错的450和505 nm荧光组成。去隔行之后,505 nm信号由具有运动伪影的Vm组成,而450 nm信号对电压的敏感度最低,并且主要包含伪影。两个信号之比估计为Vm。使用均质有限应变来量化每组3个环所包围的组织的变形。

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