Regulation of Cx36 trafficking through the early secretory pathway by COPII cargo receptors and Grasp55.

IF 6.2 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Stephan Tetenborg, Fatemeh Ariakia, Elizabeth Martinez-Soler, Eyad Shihabeddin, Ignacio Cebrian Lazart, Adam C Miller, John O'Brien
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Abstract

Gap junctions formed by the major neuronal connexin Cx36 function as electrical synapses in the nervous system and provide unique functions such as synchronizing neuron activities or supporting network oscillations. Although the physiological significance of electrical synapses for neuronal networks is well established, little is known about the pathways that regulate the transport of its main component: Cx36. Here we have used HEK293T cells as an expression system in combination with siRNA and BioID screens to study the transition of Cx36 from the ER to the cis Golgi. Our data indicate that the C-terminal tip of Cx36 is a key factor in this process, mediating binding interactions with two distinct components in the early secretory pathway: the COPII complex and the Golgi stacking protein Grasp55. The C-terminal amino acid valine serves as an ER export signal to recruit COPII cargo receptors Sec24A/B/C at ER exit sites, whereas the PDZ binding motif "SAYV" mediates an interaction with Grasp55. These two interactions have opposing effects in their respective compartments. While Sec24 subunits carry Cx36 out of the ER, Grasp55 stabilizes Cx36 in the Golgi as shown in over expression experiments. These early regulatory steps of Cx36 are expected to be essential for the formation, function, regulation and plasticity of electrical synapses in the developing and mature nervous system.

COPII 货物受体和 Grasp55 对 Cx36 通过早期分泌途径的贩运进行调控。
由主要神经元连接蛋白 Cx36 形成的间隙连接在神经系统中起着电突触的作用,并提供了独特的功能,如同步神经元活动或支持网络振荡。尽管电突触对神经元网络的生理意义已得到公认,但人们对其主要成分 Cx36 的运输调节途径却知之甚少:Cx36。在这里,我们使用 HEK293T 细胞作为表达系统,结合 siRNA 和 BioID 筛选,研究了 Cx36 从 ER 到顺式高尔基体的转变。我们的数据表明,Cx36 的 C 端是这一过程中的关键因素,它介导了与早期分泌途径中两种不同成分的结合互动:COPII 复合物和高尔基体堆积蛋白 Grasp55。C 端氨基酸缬氨酸是一种 ER 出口信号,用于在 ER 出口位点招募 COPII 货物受体 Sec24A/B/C,而 PDZ 结合基序 "SAYV "则介导与 Grasp55 的相互作用。这两种相互作用在各自的区室中产生相反的效果。Sec24 亚基将 Cx36 带出 ER,而 Grasp55 则将 Cx36 稳定在高尔基体中,正如过度表达实验所显示的那样。预计 Cx36 的这些早期调控步骤对于发育和成熟神经系统中电突触的形成、功能、调控和可塑性至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Cellular and Molecular Life Sciences
Cellular and Molecular Life Sciences 生物-生化与分子生物学
CiteScore
13.20
自引率
1.20%
发文量
546
审稿时长
1.0 months
期刊介绍: Journal Name: Cellular and Molecular Life Sciences (CMLS) Location: Basel, Switzerland Focus: Multidisciplinary journal Publishes research articles, reviews, multi-author reviews, and visions & reflections articles Coverage: Latest aspects of biological and biomedical research Areas include: Biochemistry and molecular biology Cell biology Molecular and cellular aspects of biomedicine Neuroscience Pharmacology Immunology Additional Features: Welcomes comments on any article published in CMLS Accepts suggestions for topics to be covered
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