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内源性逆转录病毒样蛋白将泛素连接酶2招募至应激颗粒并改变其功能特性。

Endogenous retrovirus-like proteins recruit UBQLN2 to stress granules and alter their functional properties.

作者信息

Mohan Harihar M, Fernandez Martin G, Huang Camellia, Lin Rita, Ryou Jaimie H, Seyfried Donald, Grotewold Nikolas, Whiteley Alexandra M, Barmada Sami J, Basrur Venkatesha, Mosalaganti Shyamal, Paulson Henry L, Sharkey Lisa M

出版信息

bioRxiv. 2024 Oct 25:2024.10.24.620053. doi: 10.1101/2024.10.24.620053.

Abstract

The human genome is replete with sequences derived from foreign elements including endogenous retrovirus-like proteins of unknown function. Here we show that UBQLN2, a ubiquitin-proteasome shuttle factor implicated in neurodegenerative diseases, is regulated by the linked actions of two retrovirus-like proteins, RTL8 and PEG10. RTL8 confers on UBQLN2 the ability to complex with and regulate PEG10. PEG10, a core component of stress granules, drives the recruitment of UBQLN2 to stress granules under various stress conditions, but can only do so when RTL8 is present. Changes in PEG10 levels further remodel the kinetics of stress granule disassembly and overall composition by incorporating select extracellular vesicle proteins. Within stress granules, PEG10 forms virus-like particles, underscoring the structural heterogeneity of this class of biomolecular condensates. Together, these results reveal an unexpected link between pathways of cellular proteostasis and endogenous retrovirus-like proteins.

摘要

人类基因组中充满了源自外来元件的序列,包括功能未知的内源性逆转录病毒样蛋白。在此我们表明,与神经退行性疾病相关的泛素-蛋白酶体穿梭因子UBQLN2受两种逆转录病毒样蛋白RTL8和PEG10的联合作用调控。RTL8赋予UBQLN2与PEG10结合并对其进行调控的能力。PEG10是应激颗粒的核心成分,在各种应激条件下驱动UBQLN2募集到应激颗粒,但只有在RTL8存在时才能做到。PEG10水平的变化通过纳入特定的细胞外囊泡蛋白,进一步重塑应激颗粒解体的动力学和整体组成。在应激颗粒内,PEG10形成病毒样颗粒,突出了这类生物分子凝聚物的结构异质性。总之,这些结果揭示了细胞蛋白质稳态途径与内源性逆转录病毒样蛋白之间意想不到的联系。

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