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心肌细胞钙诱导钙释放机制模型。

Model of calcium-induced calcium release mechanism in cardiac cells.

作者信息

Wong A Y, Fabiato A, Bassingthwaighthe J B

机构信息

Department of Physiology and Biophysics, Dalhousie University, B3H 4H7, Halifax, Nova Scotia, Canada.

出版信息

Bull Math Biol. 1992 Jan;54(1):95-116. doi: 10.1007/BF02458622.

Abstract

A model with which to elucidate the mechanism of Ca(2+) release from, and Ca(2+) loading in the sarcoplasmic reticulum (SR) by Ca(2+) current (I Ca) in cardiac cells is proposed. The SR is assumed to be comprised of three functional subcompartments: (1) the main calcium store (MCS), which contains most of the calcium (both free and bound); (2) the releasable terminal (RT), which contains the calcium readily available for release; and (3) the longitudinal network of the SR (LSR), which sequesters and the transfers the sarcoplasmic calcium to the RT. A rapid increase of the Ca(2+) concentration at the outer surface of the SR (Cae) due to the fast component of I(Ca) activates and inactivates this surface, inducing the release of Ca(2+) from the RT to the sarcoplasmic space. The RT in turn is further activated and inactivated by a increase in the concentration of sarcoplasmic Ca(2+). The Ca(2+) in the sarcoplasmic space is then sequestered by the LSR, leading to the reactivation of the RT. Further increase of Cae due to the slow component of I(Ca) enhances the entry of Ca(2+) into the MCS to be bound by the binding substance. The free Ca(2+) released from the Ca-binding substance complex is transferred to the RT for subsequent release. The activation, inactivation and reactivation are Ca(2+)-mediated and time-dependent. The proposed model yields simulation of the many events qualitatively similar to those observed experimentally in skinned cardiac cells.

摘要

提出了一个用于阐明心脏细胞中钙电流(I Ca)引起的肌浆网(SR)钙释放机制以及钙在肌浆网中负载机制的模型。假设肌浆网由三个功能亚区组成:(1)主要钙储存区(MCS),其中包含大部分钙(游离钙和结合钙);(2)可释放终末区(RT),其中含有易于释放的钙;(3)肌浆网的纵向网络(LSR),其隔离并将肌浆中的钙转运至可释放终末区。由于I(Ca)的快速成分导致肌浆网外表面钙浓度(Cae)迅速升高,激活并失活该表面,诱导钙从可释放终末区释放到肌浆空间。反过来,肌浆中钙浓度的增加进一步激活并失活可释放终末区。然后,肌浆中的钙被纵向网络隔离,导致可释放终末区重新激活。由于I(Ca)的缓慢成分导致Cae进一步升高,增强了钙进入主要钙储存区并与结合物质结合的过程。从钙结合物质复合物中释放的游离钙被转运至可释放终末区以便随后释放。激活、失活和重新激活过程是由钙介导且具有时间依赖性的。所提出的模型对许多事件的模拟在定性上与在去表皮心脏细胞中实验观察到的结果相似。

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