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篡夺与颠覆的故事:在感染与免疫的十字路口,早幼粒细胞白血病核体依赖小泛素样修饰物的完整性

A Tale of Usurpation and Subversion: SUMO-Dependent Integrity of Promyelocytic Leukemia Nuclear Bodies at the Crossroad of Infection and Immunity.

作者信息

Patra Upayan, Müller Stefan

机构信息

Institute of Biochemistry II, Faculty of Medicine, Goethe University, Frankfurt, Germany.

出版信息

Front Cell Dev Biol. 2021 Aug 27;9:696234. doi: 10.3389/fcell.2021.696234. eCollection 2021.

Abstract

Promyelocytic leukemia nuclear bodies (PML NBs) are multi-protein assemblies representing distinct sub-nuclear structures. As phase-separated molecular condensates, PML NBs exhibit liquid droplet-like consistency. A key organizer of the assembly and dynamics of PML NBs is the ubiquitin-like SUMO modification system. SUMO is covalently attached to PML and other core components of PML NBs thereby exhibiting a glue-like function by providing multivalent interactions with proteins containing SUMO interacting motifs (SIMs). PML NBs serve as the catalytic center for nuclear SUMOylation and SUMO-SIM interactions are essential for protein assembly within these structures. Importantly, however, formation of SUMO chains on PML and other PML NB-associated proteins triggers ubiquitylation and proteasomal degradation which coincide with disruption of these nuclear condensates. To date, a plethora of nuclear activities such as transcriptional and post-transcriptional regulation of gene expression, apoptosis, senescence, cell cycle control, DNA damage response, and DNA replication have been associated with PML NBs. Not surprisingly, therefore, SUMO-dependent PML NB integrity has been implicated in regulating many physiological processes including tumor suppression, metabolism, drug-resistance, development, cellular stemness, and anti-pathogen immune response. The interplay between PML NBs and viral infection is multifaceted. As a part of the cellular antiviral defense strategy, PML NB components are crucial restriction factors for many viruses and a mutual positive correlation has been found to exist between PML NBs and the interferon response. Viruses, in turn, have developed counterstrategies for disarming PML NB associated immune defense measures. On the other end of the spectrum, certain viruses are known to usurp specific PML NB components for successful replication and disruption of these sub-nuclear foci has recently been linked to the stimulation rather than curtailment of antiviral gene repertoire. Importantly, the ability of invading virions to manipulate the host SUMO modification machinery is essential for this interplay between PML NB integrity and viruses. Moreover, compelling evidence is emerging in favor of bacterial pathogens to negotiate with the SUMO system thereby modulating PML NB-directed intrinsic and innate immunity. In the current context, we will present an updated account of the dynamic intricacies between cellular PML NBs as the nuclear SUMO modification hotspots and immune regulatory mechanisms in response to viral and bacterial pathogens.

摘要

早幼粒细胞白血病核体(PML NBs)是代表不同亚核结构的多蛋白聚集体。作为相分离的分子凝聚物,PML NBs呈现出液滴状的稠度。PML NBs组装和动态变化的关键组织者是类泛素SUMO修饰系统。SUMO共价连接到PML和PML NBs的其他核心成分上,从而通过与含有SUMO相互作用基序(SIMs)的蛋白质提供多价相互作用而发挥类似胶水的功能。PML NBs作为核SUMO化的催化中心,SUMO-SIM相互作用对于这些结构内的蛋白质组装至关重要。然而,重要的是,PML和其他与PML NB相关的蛋白质上SUMO链的形成会触发泛素化和蛋白酶体降解,这与这些核凝聚物的破坏同时发生。迄今为止,大量的核活动,如基因表达的转录和转录后调控、细胞凋亡、衰老、细胞周期控制、DNA损伤反应和DNA复制,都与PML NBs有关。因此,毫不奇怪,SUMO依赖的PML NB完整性与调节许多生理过程有关,包括肿瘤抑制、代谢、耐药性、发育、细胞干性和抗病原体免疫反应。PML NBs与病毒感染之间的相互作用是多方面的。作为细胞抗病毒防御策略的一部分,PML NB成分是许多病毒的关键限制因子,并且已发现PML NBs与干扰素反应之间存在相互的正相关。反过来,病毒也制定了应对策略来解除与PML NB相关的免疫防御措施。在光谱的另一端,已知某些病毒会篡夺特定的PML NB成分以成功复制,并且最近这些亚核灶的破坏与抗病毒基因库的刺激而非抑制有关。重要的是,入侵病毒粒子操纵宿主SUMO修饰机制的能力对于PML NB完整性与病毒之间的这种相互作用至关重要。此外,越来越多的有力证据表明细菌病原体与SUMO系统相互作用,从而调节PML NB介导的固有免疫和先天免疫。在当前背景下,我们将更新关于细胞PML NBs作为核SUMO修饰热点与针对病毒和细菌病原体的免疫调节机制之间动态复杂性的阐述。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dcb1/8430037/a0174af7b350/fcell-09-696234-g001.jpg

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