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Distribution of M Cells in the Canine Ventricle

机译:M细胞在犬心室中的分布

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Distribution of M Cells.Introduction:M cells and transitional cells residing in the deep structures of the ventricular free walls are distinguished by the ability of their action potentials to prolong disproportionately to those of other ventricular cells at relatively slow rates. This feature of the M cell due, at least in part, to a smaller contribution of the slowly activating component of the delayed rectifier current (Iks) is thought to contribute to the unique pharmacologic responsiveness of M cells, making them the primary targets in ventricular myocardium lor agents that cause action potential prolongation and induce early and delayed afterdepolarizations and triggered activity. Previous studies dealt exclusively with the characteristics and distribution of M cells in the canine right and left ventricular free wall near the base of the ventricles. The present study uses standard microelectrode techniques to define their behavior and distribution in the apical region of the ventricular wall as well as in the endocardial structures of the ventricle, including the interventricular septum, papillary muscles, and trabeculae.Methods and Results:Action potentials recorded from the M region (deep subepicardium) displayed similar characteristics (steep action potential duration APD‐rate relations) in the base and apex. However, important differences were apparent in the other regions. In epicardium. (he spike and dome morphology of the action potential was less accentuated and the rate dependence of APD more pronounced in the apex versus the base. In endocardium, and especially deep subendocardium, rate dependence of APD was considerably more pronounced in the apex. Transmembrane recordings from the subsurface layers of the septum, trabeculae, and papillary muscles revealed M cell behavior (steep APD‐rate relations) in the deep subendocardium. Epicardial and transitional behavior were also observed in the deep layers of these endocardial structures.Conclusion:Our results indicate that M cells reside throughout thedeep subepicardial layers of the freewall of the canine left ventricle as well as in thedeep subendocardiat layers of the septum, papillary muscles, and trabeculae. The data also demonstrate prominent transmural as well as apicobasal gradients of phase I and phase 3 repolarization. These findings may have implications relative to our understanding of the electrocardiographs J wave, T wave, U wave, and long QTV interv
机译:M细胞的分布简介:M细胞和移行细胞位于心室游离壁的深层结构中,其特点是其动作电位能够以相对较慢的速度不成比例地延长到其他心室细胞的动作电位。M细胞的这一特征至少部分是由于延迟整流电流(Iks)的缓慢激活成分的贡献较小,被认为有助于M细胞独特的药理学反应性,使它们成为心室心肌lor药物的主要靶标,这些药物引起动作电位延长并诱导早期和延迟的后去极化和触发活性。以前的研究专门涉及靠近心室底部的犬右心室和左心室游离壁中M细胞的特征和分布。本研究使用标准微电极技术来定义它们在心室壁顶端区域以及心室心内膜结构(包括室间隔、肌和小梁)中的行为和分布。方法和结果: 从 M 区(深部心外膜)记录的动作电位在基底和顶点表现出相似的特征(陡峭的动作电位持续时间 [APD] 速率关系)。然而,其他地区也存在明显的差异。在心外膜中。(动作电位的尖峰和圆顶形态不那么突出,APD的速率依赖性在顶点与基底更明显。在心内膜,尤其是心内膜深部,APD的速率依赖性在心尖更为明显。来自隔膜、小梁和肌亚表层的跨膜记录揭示了心内膜深部的 M 细胞行为(陡峭的 APD 率关系)。在这些心内膜结构的深层中也观察到心外膜和过渡行为。结论:M细胞存在于犬左心室自由壁的心外膜深层以及隔膜、肌和小梁的心内膜深层。数据还表明,I期和3期复极化具有突出的透壁性和顶端梯度。这些发现可能对我们对心电图仪 J 波、T 波、U 波和长 QTV 间隙的理解有影响。

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