Internally tagged Vps10p-domain receptors reveal uptake of the neurotrophin BDNF.

The Journal of Biological Chemistry Pub Date : 2023-10-01 Epub Date: 2023-09-01 DOI:10.1016/j.jbc.2023.105216
Marcel Klein, Antonio Virgilio Failla, Guido Hermey
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引用次数: 0

Abstract

The Vps10p-domain (Vps10p-D) receptor family consists of Sortilin, SorLA, SorCS1, SorCS2, and SorCS3. They mediate internalization and intracellular sorting of specific cargo in various cell types, but underlying molecular determinants are incompletely understood. Deciphering the dynamic intracellular itineraries of Vps10p-D receptors is crucial for understanding their role in physiological and cytopathological processes. However, studying their spatial and temporal dynamics by live imaging has been challenging so far, as terminal tagging with fluorophores presumably impedes several of their protein interactions and thus functions. Here, we addressed the lack of appropriate tools and developed functional versions of all family members internally tagged in their ectodomains. We predict folding of the newly designed receptors by bioinformatics and show their exit from the endoplasmic reticulum. We examined their subcellular localization in immortalized cells and primary cultured neurons by immunocytochemistry and live imaging. This was, as far as known, identical to that of wt counterparts. We observed homodimerization of fluorophore-tagged SorCS2 by coimmunoprecipitation and fluorescence lifetime imaging, suggesting functional leucine-rich domains. Through ligand uptake experiments, live imaging and fluorescence lifetime imaging, we show for the first time that all Vps10p-D receptors interact with the neurotrophin brain-derived neurotrophic factor and mediate its uptake, indicating functionality of the Vps10p-Ds. In summary, we developed versions of all Vps10p-D receptors, with internal fluorophore tags that preserve several functions of the cytoplasmic and extracellular domains. These newly developed fluorophore-tagged receptors are likely to serve as powerful functional tools for accurate live studies of the individual cellular functions of Vps10p-D receptors.

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内部标记的Vps10p结构域受体揭示了神经营养因子BDNF的摄取。
Vps10p结构域(Vps10p-D)受体家族由Sortilin、SorLA、SorCS1、SorCS2和SorCS3组成。它们介导各种细胞类型中特定货物的内化和细胞内分选,但潜在的分子决定因素尚不完全清楚。破译Vps10p-D受体的动态细胞内行程对于理解它们在生理和细胞病理过程中的作用至关重要。然而,到目前为止,通过活体成像研究它们的空间和时间动力学一直具有挑战性,因为用荧光团进行末端标记可能会阻碍它们的几种蛋白质相互作用,从而阻碍它们的功能。在这里,我们解决了缺乏适当工具的问题,并开发了所有家族成员在其胞外域中内部标记的功能版本。我们通过生物信息学预测了新设计的受体的折叠,并显示了它们从内质网中的退出。我们通过免疫细胞化学和活体成像检测了它们在永生化细胞和原代培养神经元中的亚细胞定位。就目前所知,这与wt的对应物完全相同。我们通过共免疫沉淀和荧光寿命成像观察到荧光团标记的SorCS2的同源二聚,表明具有功能性富含亮氨酸的结构域。通过配体摄取实验、活体成像和荧光寿命成像,我们首次表明所有Vps10p-D受体与神经营养因子脑源性神经营养因子相互作用并介导其摄取,表明Vps10p Ds的功能。总之,我们开发了所有Vps10p-D受体的版本,其内部荧光团标签保留了细胞质和细胞外结构域的几种功能。这些新开发的荧光团标记的受体可能成为对Vps10p-D受体的个体细胞功能进行精确实时研究的强大功能工具。
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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