XBP1s Links the Unfolded Protein Response to the Molecular Architecture of Mature N-Glycans.

Mahender B Dewal, Andrew S DiChiara, Aristotelis Antonopoulos, Rebecca J Taylor, Chyleigh J Harmon, Stuart M Haslam, Anne Dell, Matthew D Shoulders
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Abstract

The molecular architecture of the mature N-glycome is dynamic, with consequences for both normal and pathologic processes. Elucidating cellular mechanisms that modulate the N-linked glycome is, therefore, crucial. The unfolded protein response (UPR) is classically responsible for maintaining proteostasis in the secretory pathway by defining levels of chaperones and quality control proteins. Here, we employ chemical biology methods for UPR regulation to show that stress-independent activation of the UPR's XBP1s transcription factor also induces a panel of N-glycan maturation-related enzymes. The downstream consequence is a distinctive shift toward specific hybrid and complex N-glycans on N-glycoproteins produced from XBP1s-activated cells, which we characterize by mass spectrometry. Pulse-chase studies attribute this shift specifically to altered N-glycan processing, rather than to changes in degradation or secretion rates. Our findings implicate XBP1s in a new role for N-glycoprotein biosynthesis, unveiling an important link between intracellular stress responses and the molecular architecture of extracellular N-glycoproteins.

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XBP1s 将未折叠蛋白反应与成熟 N-聚糖的分子结构联系起来。
成熟 N-糖蛋白的分子结构是动态的,对正常和病理过程都有影响。因此,阐明调节 N-连接糖蛋白的细胞机制至关重要。未折叠蛋白反应(UPR)通过确定伴侣蛋白和质控蛋白的水平来维持分泌途径中的蛋白稳态。在这里,我们采用化学生物学方法对 UPR 进行调控,结果表明,与应激无关的 UPR XBP1s 转录因子的激活也会诱导一系列与 N-糖成熟相关的酶。其下游结果是,从 XBP1s 激活的细胞中产生的 N-糖蛋白上出现了向特定混合型和复合型 N-糖的独特转变,我们通过质谱法对其进行了表征。脉冲追逐研究将这种转变归因于 N-聚糖加工的改变,而不是降解或分泌率的变化。我们的研究结果揭示了 XBP1s 在 N-糖蛋白生物合成中的新作用,揭示了细胞内应激反应与细胞外 N-糖蛋白分子结构之间的重要联系。
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
Chemistry & biology
Chemistry & biology 生物-生化与分子生物学
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4-8 weeks
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