Arf1-dependent LRBA recruitment to Rab4 endosomes is required for endolysosome homeostasis.

IF 7.4 1区 生物学 Q1 CELL BIOLOGY
Viktória Szentgyörgyi,Leon Maximilian Lueck,Daan Overwijn,Danilo Ritz,Nadja Zoeller,Alexander Schmidt,Maria Hondele,Anne Spang,Shahrzad Bakhtiar
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引用次数: 0

Abstract

Deleterious mutations in the lipopolysaccharide responsive beige-like anchor protein (LRBA) gene cause severe childhood immune dysregulation. The complexity of the symptoms involving multiple organs and the broad range of unpredictable clinical manifestations of LRBA deficiency complicate the choice of therapeutic interventions. Although LRBA has been linked to Rab11-dependent trafficking of the immune checkpoint protein CTLA-4, its precise cellular role remains elusive. We show that LRBA, however, only slightly colocalizes with Rab11. Instead, LRBA is recruited by members of the small GTPase Arf protein family to the TGN and to Rab4+ endosomes, where it controls intracellular traffic. In patient-derived fibroblasts, loss of LRBA led to defects in the endosomal pathway promoting the accumulation of enlarged endolysosomes and lysosome secretion. Thus, LRBA appears to regulate flow through the endosomal system on Rab4+ endosomes. Our data strongly suggest functions of LRBA beyond CTLA-4 trafficking and provide a conceptual framework to develop new therapies for LRBA deficiency.
内溶酶体稳态需要 Arf1 依赖性 LRBA 招募到 Rab4 内体。
脂多糖反应性米色样锚蛋白(LRBA)基因的畸变会导致严重的儿童免疫失调。LRBA 缺乏症的症状复杂,涉及多个器官,临床表现多种多样,难以预测,这使得治疗干预措施的选择变得复杂。虽然 LRBA 与依赖 Rab11 的免疫检查点蛋白 CTLA-4 的转运有关,但其在细胞中的确切作用仍然难以捉摸。然而,我们发现 LRBA 只与 Rab11 稍微共定位。相反,LRBA 被小 GTPase Arf 蛋白家族成员招募到 TGN 和 Rab4+ 内体,并在那里控制细胞内的运输。在患者来源的成纤维细胞中,LRBA 的缺失会导致内体通路的缺陷,促进增大的内溶酶体的积累和溶酶体的分泌。因此,LRBA 似乎能调节 Rab4+ 内体上通过内体系统的流量。我们的数据有力地证明了 LRBA 在 CTLA-4 转运之外的功能,并为开发治疗 LRBA 缺乏症的新疗法提供了一个概念框架。
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来源期刊
Journal of Cell Biology
Journal of Cell Biology 生物-细胞生物学
CiteScore
12.60
自引率
2.60%
发文量
213
审稿时长
1 months
期刊介绍: The Journal of Cell Biology (JCB) is a comprehensive journal dedicated to publishing original discoveries across all realms of cell biology. We invite papers presenting novel cellular or molecular advancements in various domains of basic cell biology, along with applied cell biology research in diverse systems such as immunology, neurobiology, metabolism, virology, developmental biology, and plant biology. We enthusiastically welcome submissions showcasing significant findings of interest to cell biologists, irrespective of the experimental approach.
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