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首页> 外文期刊>American Journal of Physiology >Heterogeneity of action potential durations in isolated mouse left and right atria recorded using voltage-sensitive dye mapping.
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Heterogeneity of action potential durations in isolated mouse left and right atria recorded using voltage-sensitive dye mapping.

机译:使用电压敏感染料图谱记录孤立小鼠左,右心房中动作电位持续时间的异质性。

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An imaging system for di-4-ANEPPS (4-[beta-[2-(di-n-butylamino)-6-naphthylvinyl]pyridinium]) voltage-sensitive dye recordings has been adapted for recording from an in vitro mouse heart preparation that consists of both atria in isolation. This approach has been used to study inter- and intra-atrial activation and conduction and to monitor action potential durations (APDs) in the left and right atrium. The findings from this study confirm some of our previous findings in isolated mouse atrial myocytes and demonstrate that many electrophysiological properties of mouse atria closely resemble those of larger mammals. Specifically, we made the following observations: 1) Activation in mouse atria originates in the sinoatrial node and spreads into the right atrium and, after a delay, into the left atrium. 2) APD in the left atrium is shorter than in the right atrium. 3) Sites in the posterior walls have longer APDs than sites in the atrial appendages. 4) Superfusion of this preparation with 4-aminopyridine and tetraethylammonium resulted in increases in APD, consistent with their inhibitory effects on the K+ currents known to be expressed in mouse atria. 5) The muscarinic agonist carbachol shortened APD in all areas of the preparation, except the left atrial appendage, in which carbachol had no statistically significant effect on APD. These results validate a new approach for monitoring activation, conduction, and repolarization in mouse atria and demonstrate that the physiological and pharmacological properties of mouse atria are sufficiently similar to those of larger animals to warrant further studies using this preparation.
机译:二-4-ANEPPS(4- [β-[2-(二-正丁基氨基)-6-萘乙烯基]吡啶])电压敏感染料记录的成像系统已适应于从体外小鼠心脏制备物中进行记录由两个孤立的心房组成。该方法已用于研究房间和房内的激活和传导,并监测左心房和右心房的动作电位持续时间(APD)。这项研究的结果证实了我们先前在分离的小鼠心房肌细胞中的一些发现,并证明了小鼠心房的许多电生理特性与较大的哺乳动物的生理特性非常相似。具体来说,我们进行了以下观察:1)小鼠心房的激活起源于窦房结,并扩散到右心房,并在延迟后扩散到左心房。 2)左心房的APD短于右心房。 3)后壁部位的APD比心房附件的部位更长。 4)该制剂与4-氨基吡啶和四乙铵的过量混入导致APD的增加,这与它们对已知在小鼠心房中表达的K +电流的抑制作用一致。 5)毒蕈碱激动剂卡巴胆碱在制剂的所有区域均缩短了APD,左心耳除外,其中左卡巴胆碱对APD没有统计学意义。这些结果验证了一种监测小鼠心房激活,传导和复极化的新方法,并证明了小鼠心房的生理和药理特性与较大动物的生理和药理特性足够相似,因此有必要使用该制剂进行进一步研究。

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