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心脏组织中的起搏。从IK2到耦合时钟系统。

Pacemaking in cardiac tissue. From IK2 to a coupled-clock system.

作者信息

Carmeliet Edward

机构信息

Katholieke Universiteit Leuven, Leuven, Belgium.

出版信息

Physiol Rep. 2019 Jan;7(1):e13862. doi: 10.14814/phy2.13862.

Abstract

Initially, diastolic depolarization in Purkinje fibers was explained by deactivation of gK2 in the presence of inward current. Weakness of the hypothesis was a too negative reversal potential, sensitivity to external Na ions, existence of K depletion, and fake current during hyperpolarizing clamps. The development of a sinus node preparation of almost microscopic dimensions allowing uniform voltage clamps created new possibilities. Three different groups discovered in this improved node preparation an hyperpolarization induced time-dependent inward current, with a reversal potential positive to the resting potential, carried by a mixture of Na and K ions. A new current, If, or funny current was born. It is not the only pacemaker current. The following sequence of currents (membrane clock) has been proposed: diastole starts as a consequence of IK deactivation and If activation; followed by activation of the T-type Ca current, Ca -induced Ca release from the SR, and activation of sodium-calcium exchange current with further depolarization of the membrane till threshold of the L-type Ca current is reached. The release of Ca can also occur spontaneously independently from a T-type Ca current. The system acts then as a primary intracellular clock. The review is completed by description of an evolution in the direction of biological pacing using induced pluripotent stem cells or transcription factors. See also: https://doi.org/10.14814/phy2.13860 & https://doi.org/10.14814/phy2.13861.

摘要

最初,浦肯野纤维的舒张期去极化是通过内向电流存在时gK2的失活来解释的。该假说的不足之处在于反转电位过于负、对外部钠离子敏感、存在钾离子耗竭以及超极化钳制期间的假电流。几乎微观尺寸的窦房结标本的发展使得均匀电压钳制成为可能。在这种改进的窦房结标本中,三个不同的研究小组发现了一种超极化诱导的时间依赖性内向电流,其反转电位相对于静息电位为正,由钠和钾离子的混合物携带。一种新的电流,If,即“趣电流”诞生了。它并不是唯一的起搏电流。有人提出了以下电流序列(膜时钟):舒张期开始于IK失活和If激活;随后是T型钙电流的激活、钙从肌浆网的钙诱导释放以及钠钙交换电流的激活,随着膜进一步去极化直至达到L型钙电流的阈值。钙的释放也可以独立于T型钙电流自发发生。然后该系统作为主要的细胞内时钟起作用。本文通过描述使用诱导多能干细胞或转录因子在生物起搏方向上的进展来完成综述。另见:https://doi.org/10.14814/phy2.13860 & https://doi.org/10.14814/phy2.13861

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7bb0/6317064/a01be8bb78e4/PHY2-7-e13862-g001.jpg

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