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钙调蛋白结合蛋白在心肌细胞中提供局部 Ca2+信号的结构域。

Calmodulin binding proteins provide domains of local Ca2+ signaling in cardiac myocytes.

机构信息

Department of Biomedical Engineering, Robert M. Berne Cardiovascular Research Center, University of Virginia, Charlottesville, VA 22908, USA.

出版信息

J Mol Cell Cardiol. 2012 Feb;52(2):312-6. doi: 10.1016/j.yjmcc.2011.06.005. Epub 2011 Jun 12.

Abstract

Calmodulin (CaM) acts as a common Ca(2+) sensor for many signaling pathways, transducing local Ca(2+) signals into specific cellular outcomes. Many of CaM's signaling functions can be explained by its unique biochemical properties, including high and low affinity Ca(2+)-binding sites with slow and fast kinetics, respectively. CaM is expected to have a limited spatial range of action, emphasizing its role in local Ca(2+) signaling. Interactions with target proteins further fine-tune CaM signal transduction. Here, we focus on only three specific cellular targets for CaM signaling in cardiac myocytes: the L-type Ca(2+) channel, the ryanodine receptor, and the IP(3) receptor. We elaborate a working hypothesis that each channel is regulated by two distinct functional populations of CaM: dedicated CaM and promiscuous CaM. Dedicated CaM is typically tethered to each channel and directly regulates channel activity. In addition, a local pool of promiscuous CaM appears poised to sense local Ca(2+) signals and trigger downstream pathways such as Ca(2+)/CaM dependent-protein kinase II and calcineurin. Understanding how promiscuous CaM coordinates multiple distinct signaling pathways remains a challenge, but is aided by the use of mathematical modeling and a new generation of fluorescent biosensors. This article is part of a special issue entitled "Local Signaling in Myocytes."

摘要

钙调蛋白(CaM)作为许多信号通路的通用 Ca(2+)传感器,将局部 Ca(2+)信号转导为特定的细胞效应。CaM 的许多信号功能可以用其独特的生化特性来解释,包括具有慢和快动力学的高亲和和低亲和 Ca(2+)-结合位点。CaM 的作用空间范围预计有限,强调其在局部 Ca(2+)信号转导中的作用。与靶蛋白的相互作用进一步微调 CaM 信号转导。在这里,我们仅关注心肌细胞中 CaM 信号的三个特定细胞靶标:L 型 Ca(2+)通道、兰尼碱受体和 IP(3)受体。我们详细阐述了一个工作假设,即每个通道都由两种不同的 CaM 功能群调节:专用 CaM 和混杂 CaM。专用 CaM 通常与每个通道相连,并直接调节通道活性。此外,局部混杂 CaM 池似乎准备好感知局部 Ca(2+)信号并触发下游途径,如 Ca(2+)/CaM 依赖性蛋白激酶 II 和钙调神经磷酸酶。了解混杂 CaM 如何协调多个不同的信号通路仍然是一个挑战,但数学建模和新一代荧光生物传感器的使用有助于解决这一问题。本文是题为“心肌细胞中的局部信号”的特刊的一部分。

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