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TRP 储存操纵通道定位于信号复合物所需的 PDZ 结构域蛋白 INAD。

Requirement for the PDZ domain protein, INAD, for localization of the TRP store-operated channel to a signaling complex.

作者信息

Chevesich J, Kreuz A J, Montell C

机构信息

Department of Biological Chemistry, The Johns Hopkins University School of Medicine, Baltimore, Maryland 21205, USA.

出版信息

Neuron. 1997 Jan;18(1):95-105. doi: 10.1016/s0896-6273(01)80049-0.

Abstract

In Drosophila, the store-operated Ca2+ channel, TRP, is required in photoreceptor cells for a sustained response to light. Here, we show that TRP forms a complex with phospholipase C-beta (NORPA), rhodopsin (RH1), calmodulin, and the PDZ domain containing protein INAD. Proteins with PDZ domains have previously been shown to cluster ion channels in vitro. We show that in InaD mutant flies, TRP is no longer spatially restricted to its normal subcellular compartment, the rhabdomere. These results provide evidence that a PDZ domain protein is required, in vivo, for anchoring of an ion channel to a signaling complex. Furthermore, disruption of this interaction results in retinal degeneration. We propose that the TRP channel is linked to NORPA and RH1 to facilitate feedback regulation of these upstream signaling molecules.

摘要

在果蝇中,光感受器细胞对光的持续反应需要储存式钙离子通道TRP。在此,我们表明TRP与磷脂酶C-β(NORPA)、视紫红质(RH1)、钙调蛋白以及含PDZ结构域的蛋白INAD形成复合物。先前已证明含PDZ结构域的蛋白在体外可使离子通道聚集。我们表明,在InaD突变果蝇中,TRP不再在空间上局限于其正常的亚细胞区室——微绒毛。这些结果提供了证据,证明在体内需要一种PDZ结构域蛋白将离子通道锚定到信号复合物上。此外,这种相互作用的破坏会导致视网膜退化。我们提出,TRP通道与NORPA和RH1相连,以促进对这些上游信号分子的反馈调节。

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