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秀丽隐杆线虫 junctophilin 具有组织特异性功能,并与延伸突触结合蛋白一起调节神经递质传递。

Caenorhabditis elegans junctophilin has tissue-specific functions and regulates neurotransmission with extended-synaptotagmin.

机构信息

Section of Neurobiology, Division of Biological Sciences, University of California San Diego, La Jolla, CA 92093, USA.

Department of Molecular Biology, Massachusetts General Hospital, Boston, MA 02114, USA.

出版信息

Genetics. 2021 Aug 9;218(4). doi: 10.1093/genetics/iyab063.

Abstract

The junctophilin family of proteins tether together plasma membrane (PM) and endoplasmic reticulum (ER) membranes, and couple PM- and ER-localized calcium channels. Understanding in vivo functions of junctophilins is of great interest for dissecting the physiological roles of ER-PM contact sites. Here, we show that the sole Caenorhabditis elegans junctophilin JPH-1 localizes to discrete membrane contact sites in neurons and muscles and has important tissue-specific functions. jph-1 null mutants display slow growth and development due to weaker contraction of pharyngeal muscles, leading to reduced feeding. In the body wall muscle, JPH-1 colocalizes with the PM-localized EGL-19 voltage-gated calcium channel and ER-localized UNC-68 RyR calcium channel, and is required for animal movement. In neurons, JPH-1 colocalizes with the membrane contact site protein Extended-SYnaptoTagmin 2 (ESYT-2) in the soma, and is present near presynaptic release sites. Interestingly, jph-1 and esyt-2 null mutants display mutual suppression in their response to aldicarb, suggesting that JPH-1 and ESYT-2 have antagonistic roles in neuromuscular synaptic transmission. Additionally, we find an unexpected cell nonautonomous effect of jph-1 in axon regrowth after injury. Genetic double mutant analysis suggests that jph-1 functions in overlapping pathways with two PM-localized voltage-gated calcium channels, egl-19 and unc-2, and with unc-68 for animal health and development. Finally, we show that jph-1 regulates the colocalization of EGL-19 and UNC-68 and that unc-68 is required for JPH-1 localization to ER-PM puncta. Our data demonstrate important roles for junctophilin in cellular physiology, and also provide insights into how junctophilin functions together with other calcium channels in vivo.

摘要

衔接蛋白家族将质膜 (PM) 和内质网 (ER) 膜连接在一起,并将 PM 和 ER 定位的钙通道连接起来。了解衔接蛋白的体内功能对于剖析 ER-PM 接触位点的生理作用非常重要。在这里,我们表明,秀丽隐杆线虫中唯一的衔接蛋白 JPH-1 定位于神经元和肌肉中的离散膜接触位点,并且具有重要的组织特异性功能。jph-1 缺失突变体由于咽肌收缩较弱而导致生长和发育缓慢,从而导致摄食减少。在体壁肌肉中,JPH-1 与 PM 定位的 EGL-19 电压门控钙通道和 ER 定位的 UNC-68 RyR 钙通道共定位,并且是动物运动所必需的。在神经元中,JPH-1 与膜接触位点蛋白 Extended-SYnaptoTagmin 2 (ESYT-2) 在体部共定位,并且存在于突触前释放位点附近。有趣的是,jph-1 和 esyt-2 缺失突变体在对 aldicarb 的反应中表现出相互抑制,表明 JPH-1 和 ESYT-2 在神经肌肉突触传递中具有拮抗作用。此外,我们发现 jph-1 在损伤后轴突再生中存在意想不到的细胞非自主性效应。遗传双突变体分析表明,jph-1 与两个 PM 定位的电压门控钙通道 egl-19 和 unc-2 以及 unc-68 在功能上重叠,而 unc-68 对动物的健康和发育是必需的。最后,我们表明 jph-1 调节 EGL-19 和 UNC-68 的共定位,并且 unc-68 是 JPH-1 定位于 ER-PM 点状结构所必需的。我们的数据表明衔接蛋白在细胞生理学中具有重要作用,并为了解衔接蛋白在体内与其他钙通道一起发挥作用提供了新的见解。

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