Song Long-Sheng, Guatimosim Silvia, Gómez-Viquez Leticia, Sobie Eric A, Ziman Andrew, Hartmann Hali, Lederer W J
Medical Biotechnology Center and the Institute of Molecular Cardiology, University of Maryland Biotechnology Institute, Baltimore, Maryland 21201, USA.
Ann N Y Acad Sci. 2005 Jun;1047:99-111. doi: 10.1196/annals.1341.009.
Ca(2+) sparks in heart muscle are activated on depolarization by the influx of Ca(2+) through dihydropyridine receptors in the sarcolemmal (SL) and transverse tubule (TT) membranes. The cardiac action potential is thus able to synchronize the Ca(2+) transient as Ca(2+) release is activated throughout the cell. Increases in the amount of Ca(2+) within the sarcoplasmic reticulum (SR) underlie augmented Ca(2+) release globally and an increase in the sensitivity of the ryanodine receptors (RyRs) to be triggered by the local Ca(2+). In a similar manner, phosphorylation of the RyRs by protein kinase A (PKA) increases the sensitivity of the RyRs to be activated by local Ca(2+). Heart failure and other cardiac diseases are associated with changes in SR Ca(2+) content, phosphorylation state of the RyRs, Ca(2+) signaling defects and arrhythmias. Additional changes in transverse tubules and nearby junctional SR may contribute to alterations in local Ca(2+) signaling. Here we briefly discuss how TT organization can influence Ca(2+) signaling and how changes in SR Ca(2+) release triggering can influence excitation-contraction (EC) coupling. High speed imaging methods are used in combination with single cell patch clamp experiments to investigate how abnormal Ca(2+) signaling may be regulated in health and disease. Three issues are examined in this presentation: (1) normal Ca(2+)-induced Ca(2+) release and Ca(2+) sparks, (2) abnormal SR Ca(2+) release in disease, and (3) the triggering and propagation of waves of elevated Ca(2+).
心肌中的Ca(2+)火花在去极化时被激活,此时Ca(2+)通过肌膜(SL)和横管(TT)膜中的二氢吡啶受体流入。因此,心脏动作电位能够使[Ca(2+)]i瞬变同步,因为Ca(2+)释放会在整个细胞中被激活。肌浆网(SR)内Ca(2+)量的增加是全球范围内Ca(2+)释放增强以及兰尼碱受体(RyRs)对局部[Ca(2+)]i触发敏感性增加的基础。以类似的方式,蛋白激酶A(PKA)对RyRs的磷酸化增加了RyRs被局部[Ca(2+)]i激活的敏感性。心力衰竭和其他心脏疾病与SR Ca(2+)含量的变化、RyRs的磷酸化状态、[Ca(2+)]i信号缺陷和心律失常有关。横管和附近连接SR的其他变化可能导致局部Ca(2+)信号的改变。在这里,我们简要讨论TT组织如何影响Ca(2+)信号,以及SR Ca(2+)释放触发的变化如何影响兴奋-收缩(EC)偶联。高速成像方法与单细胞膜片钳实验相结合,用于研究健康和疾病状态下异常Ca(2+)信号可能如何被调节。本报告中研究了三个问题:(1)正常的Ca(2+)诱导的Ca(2+)释放和Ca(2+)火花,(2)疾病中异常的SR Ca(2+)释放,以及(3)[Ca(2+)]i升高波的触发和传播。