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锌离子和铜离子对泛病毒核衣壳生物分子凝聚物的类朊病毒液-液相分离动力学具有差异调节作用。

Zinc and Copper Ions Differentially Regulate Prion-Like Phase Separation Dynamics of Pan-Virus Nucleocapsid Biomolecular Condensates.

机构信息

Lady Davis Institute at the Jewish General Hospital, Montréal, QC H3T 1E2, Canada.

Department of Medicine, McGill University, Montréal, QC H4A 3J1, Canada.

出版信息

Viruses. 2020 Oct 18;12(10):1179. doi: 10.3390/v12101179.

Abstract

Liquid-liquid phase separation (LLPS) is a rapidly growing research focus due to numerous demonstrations that many cellular proteins phase-separate to form biomolecular condensates (BMCs) that nucleate membraneless organelles (MLOs). A growing repertoire of mechanisms supporting BMC formation, composition, dynamics, and functions are becoming elucidated. BMCs are now appreciated as required for several steps of gene regulation, while their deregulation promotes pathological aggregates, such as stress granules (SGs) and insoluble irreversible plaques that are hallmarks of neurodegenerative diseases. Treatment of BMC-related diseases will greatly benefit from identification of therapeutics preventing pathological aggregates while sparing BMCs required for cellular functions. Numerous viruses that block SG assembly also utilize or engineer BMCs for their replication. While BMC formation first depends on prion-like disordered protein domains (PrLDs), metal ion-controlled RNA-binding domains (RBDs) also orchestrate their formation. Virus replication and viral genomic RNA (vRNA) packaging dynamics involving nucleocapsid (NC) proteins and their orthologs rely on Zinc (Zn) availability, while virus morphology and infectivity are negatively influenced by excess Copper (Cu). While virus infections modify physiological metal homeostasis towards an increased copper to zinc ratio (Cu/Zn), how and why they do this remains elusive. Following our recent finding that pan-retroviruses employ Zn for NC-mediated LLPS for virus assembly, we present a pan-virus bioinformatics and literature meta-analysis study identifying metal-based mechanisms linking virus-induced BMCs to neurodegenerative disease processes. We discover that conserved degree and placement of PrLDs juxtaposing metal-regulated RBDs are associated with disease-causing prion-like proteins and are common features of viral proteins responsible for virus capsid assembly and structure. Virus infections both modulate gene expression of metalloproteins and interfere with metal homeostasis, representing an additional virus strategy impeding physiological and cellular antiviral responses. Our analyses reveal that metal-coordinated virus NC protein PrLDs initiate LLPS that nucleate pan-virus assembly and contribute to their persistence as cell-free infectious aerosol droplets. Virus aerosol droplets and insoluble neurological disease aggregates should be eliminated by physiological or environmental metals that outcompete PrLD-bound metals. While environmental metals can control virus spreading via aerosol droplets, therapeutic interference with metals or metalloproteins represent additional attractive avenues against pan-virus infection and virus-exacerbated neurological diseases.

摘要

液-液相分离(LLPS)是一个快速发展的研究焦点,因为有大量的证据表明,许多细胞蛋白相分离形成生物分子凝聚物(BMCs),从而形成无膜细胞器(MLOs)。越来越多的支持 BMC 形成、组成、动态和功能的机制正在被阐明。BMCs 现在被认为是基因调控的几个步骤所必需的,而它们的失调会促进病理聚集物的形成,如应激颗粒(SGs)和不可溶性不可逆斑块,这些都是神经退行性疾病的标志。治疗与 BMC 相关的疾病将大大受益于识别出既能阻止病理聚集物又能保留细胞功能所需的 BMC 的治疗方法。许多阻止 SG 组装的病毒也利用或设计 BMC 进行复制。虽然 BMC 的形成首先依赖于类朊病毒无序蛋白结构域(PrLDs),但金属离子控制的 RNA 结合结构域(RBDs)也可以协调它们的形成。涉及核衣壳(NC)蛋白及其同源物的病毒复制和病毒基因组 RNA(vRNA)包装动力学依赖于锌(Zn)的可用性,而病毒形态和感染性则受到过量铜(Cu)的负面影响。尽管病毒感染会使生理金属稳态向增加铜锌比(Cu/Zn)的方向改变,但它们为什么会这样做仍然难以捉摸。在我们最近发现泛逆转录病毒利用 NC 介导的 LLPS 进行病毒组装的锌之后,我们提出了一项泛病毒生物信息学和文献荟萃分析研究,确定了将病毒诱导的 BMC 与神经退行性疾病过程联系起来的基于金属的机制。我们发现,PrLDs 与金属调控的 RBDs 相邻的保守程度和位置与导致疾病的类朊病毒蛋白有关,是负责病毒衣壳组装和结构的病毒蛋白的共同特征。病毒感染不仅调节金属蛋白酶的基因表达,还干扰金属稳态,这是病毒阻止生理和细胞抗病毒反应的另一种策略。我们的分析表明,金属协调的病毒 NC 蛋白 PrLDs 启动 LLPS,从而引发泛病毒组装,并有助于它们作为无细胞感染性气溶胶液滴的持续存在。生理或环境金属可以替代 PrLD 结合的金属,从而消除病毒气溶胶液滴和不可溶性神经疾病聚集物。虽然环境金属可以通过气溶胶液滴控制病毒的传播,但通过干扰金属或金属蛋白酶进行治疗是对抗泛病毒感染和病毒加剧的神经退行性疾病的另一种有吸引力的途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/47de/7589941/7c83a38d8ed4/viruses-12-01179-g001.jpg

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