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ISGylation- 锁定细胞大门的关键,以防止威胁的传播。

ISGylation - a key to lock the cell gates for preventing the spread of threats.

机构信息

Vascular Pathophysiology Area, Centro Nacional de Investigaciones Cardiovasculares (CNIC), 28029 Madrid, Spain.

Immunology Service, Hospital de la Princesa, Universidad Autónoma de Madrid, 28006 Madrid, Spain.

出版信息

J Cell Sci. 2017 Sep 15;130(18):2961-2969. doi: 10.1242/jcs.205468. Epub 2017 Aug 25.

Abstract

Interferon stimulated gene 15 (ISG15) is an ubiquitin-like protein whose expression and conjugation to targets (ISGylation) is induced by infection, interferon (IFN)-α and -β, ischemia, DNA damage and aging. Attention has historically focused on the antiviral effects of ISGylation, which blocks the entry, replication or release of different intracellular pathogens. However, recently, new functions of ISGylation have emerged that implicate it in multiple cellular processes, such as DNA repair, autophagy, protein translation and exosome secretion. In this Review, we discuss the induction and conjugation of ISG15, as well as the functions of ISGylation in the prevention of infections and in cancer progression. We also offer a novel perspective with regard to the latest findings on this pathway, with special attention to the role of ISGylation in the inhibition of exosome secretion, which is mediated by fusion of multivesicular bodies with lysosomes. Finally, we propose that under conditions of stress or infection, ISGylation acts as a defense mechanism to inhibit normal protein translation by modifying protein kinase R (PKR, also known as EIF2AK2), while any newly synthesized proteins are being tagged and thus marked as potentially dangerous. Then, the endosomal system is re-directed towards protein degradation at the lysosome, to effectively 'lock' the cell gates and thus prevent the spread of pathogens, prions and deleterious aggregates through exosomes.

摘要

干扰素刺激基因 15(ISG15)是一种泛素样蛋白,其表达和与靶标的缀合(ISGylation)可被感染、干扰素(IFN)-α 和 -β、缺血、DNA 损伤和衰老所诱导。历史上,人们一直关注 ISGylation 的抗病毒作用,它可以阻止不同的细胞内病原体的进入、复制或释放。然而,最近,ISGylation 的新功能已经出现,表明它参与了多种细胞过程,如 DNA 修复、自噬、蛋白质翻译和外泌体分泌。在这篇综述中,我们讨论了 ISG15 的诱导和缀合,以及 ISGylation 在预防感染和癌症进展中的作用。我们还提供了关于该途径最新发现的新视角,特别关注 ISGylation 在抑制外泌体分泌中的作用,这种作用是通过多泡体与溶酶体融合介导的。最后,我们提出,在应激或感染条件下,ISGylation 作为一种防御机制,通过修饰蛋白激酶 R(PKR,也称为 EIF2AK2)来抑制正常的蛋白质翻译,而任何新合成的蛋白质都被标记,因此被视为潜在的危险。然后,内体系统被重新导向溶酶体进行蛋白质降解,有效地“锁定”细胞门,从而防止病原体、朊病毒和有害聚集体通过外泌体传播。

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