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大鼠脑中二氢吡啶受体与1型兰尼碱受体的分子相互作用。

Molecular interaction of dihydropyridine receptors with type-1 ryanodine receptors in rat brain.

作者信息

Mouton J, Marty I, Villaz M, Feltz A, Maulet Y

机构信息

Laboratoire de Neurobiologie Cellulaire, CNRS, 5 rue Blaise Pascal, 67084 Strasbourg, France.

出版信息

Biochem J. 2001 Mar 15;354(Pt 3):597-603. doi: 10.1042/0264-6021:3540597.

Abstract

In striated muscles, Ca2+ release from internal stores through ryanodine receptor (RyR) channels is triggered by functional coupling to voltage-activated Ca2+ channels known as dihydropyridine receptors (DHPRs) located in the plasma membrane. In skeletal muscle, this occurs by a direct conformational link between the tissue-specific DHPR (Ca(v)1.1) and RyR(1), whereas in the heart the signal is carried from the cardiac-type DHPR (Ca(v)1.2) to RyR(2) by calcium ions acting as an activator. Subtypes of both channels are expressed in the central nervous system, but their functions and mechanisms of coupling are still poorly understood. We show here that complexes immunoprecipitated from solubilized rat brain membranes with antibodies against DHPR of the Ca(v)1.2 or Ca(v)1.3 subtypes contain RyR. Only type-1 RyR is co-precipitated, although the major brain isoform is RyR(2). This suggests that, in neurons, DHPRs could communicate with RyRs by way of a strong molecular interaction and, more generally, that the physical link between DHPR and RyR shown to exist in skeletal muscle can be extended to other tissues.

摘要

在横纹肌中,通过位于质膜上的被称为二氢吡啶受体(DHPRs)的电压激活钙通道的功能偶联,触发内部储存的Ca2+通过兰尼碱受体(RyR)通道释放。在骨骼肌中,这是通过组织特异性DHPR(Ca(v)1.1)和RyR(1)之间的直接构象联系发生的,而在心脏中,信号通过作为激活剂的钙离子从心脏型DHPR(Ca(v)1.2)传递到RyR(2)。这两种通道的亚型都在中枢神经系统中表达,但其功能和偶联机制仍知之甚少。我们在此表明,用针对Ca(v)1.2或Ca(v)1.3亚型的DHPR的抗体从溶解的大鼠脑膜中免疫沉淀的复合物含有RyR。尽管主要的脑亚型是RyR(2),但只有1型RyR被共沉淀。这表明,在神经元中,DHPRs可能通过强烈的分子相互作用与RyRs进行通讯,更普遍地说,骨骼肌中显示存在的DHPR和RyR之间的物理联系可以扩展到其他组织。

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