Subramani Chandru, Nair Vidya P, Anang Saumya, Mandal Sukhen Das, Pareek Madhu, Kaushik Nidhi, Srivastava Akriti, Saha Sudipto, Nayak Baibaswata, Ranjith-Kumar C T, Surjit Milan
Virology Laboratory, Vaccine and Infectious Disease Research Centre, Translational Health Science and Technology Institute, NCR Biotech Science Cluster, 3rd Milestone, Faridabad-Gurgaon Expressway, Faridabad, Haryana, India.
Bioinformatics Centre, Bose Institute, Kolkata, West Bengal, India.
mSystems. 2018 Jan 23;3(1). doi: 10.1128/mSystems.00135-17. eCollection 2018 Jan-Feb.
Comprehensive knowledge of host-pathogen interactions is central to understand the life cycle of a pathogen and devise specific therapeutic strategies. Protein-protein interactions (PPIs) are key mediators of host-pathogen interactions. Hepatitis E virus (HEV) is a major cause of viral hepatitis in humans. Recent reports also demonstrate its extrahepatic manifestations in the brain. Toward understanding the molecular details of HEV life cycle, we screened human liver and fetal brain cDNA libraries to identify the host interaction partners of proteins encoded by genotype 1 HEV and constructed the virus-host PPI network. Analysis of the network indicated a role of HEV proteins in modulating multiple host biological processes such as stress and immune responses, the ubiquitin-proteasome system, energy and iron metabolism, and protein translation. Further investigations revealed the presence of multiple host translation regulatory factors in the viral translation/replication complex. Depletion of host translation factors such as eIF4A2, eIF3A, and RACK1 significantly reduced the viral replication, whereas eIF2AK4 depletion had no effect. These findings highlight the ingenuity of the pathogen in manipulating the host machinery to its own benefit, a clear understanding of which is essential for the identification of strategic targets and development of specific antivirals against HEV. Hepatitis E virus (HEV) is a pathogen that is transmitted by the fecal-oral route. Owing to the lack of an efficient laboratory model, the life cycle of the virus is poorly understood. During the course of infection, interactions between the viral and host proteins play essential roles, a clear understanding of which is essential to decode the life cycle of the virus. In this study, we identified the direct host interaction partners of all HEV proteins and generated a PPI network. Our functional analysis of the HEV-human PPI network reveals a role of HEV proteins in modulating multiple host biological processes such as stress and immune responses, the ubiquitin-proteasome system, energy and iron metabolism, and protein translation. Further investigations revealed an essential role of several host factors in HEV replication. Collectively, the results from our study provide a vast resource of PPI data from HEV and its human host and identify the molecular components of the viral translation/replication machinery.
全面了解宿主与病原体的相互作用对于理解病原体的生命周期和制定特定的治疗策略至关重要。蛋白质-蛋白质相互作用(PPI)是宿主与病原体相互作用的关键介质。戊型肝炎病毒(HEV)是人类病毒性肝炎的主要病因。最近的报告还表明其在大脑中有肝外表现。为了了解HEV生命周期的分子细节,我们筛选了人类肝脏和胎儿脑cDNA文库,以鉴定1型HEV编码蛋白的宿主相互作用伙伴,并构建了病毒-宿主PPI网络。对该网络的分析表明,HEV蛋白在调节多种宿主生物学过程中发挥作用,如应激和免疫反应、泛素-蛋白酶体系统、能量和铁代谢以及蛋白质翻译。进一步的研究揭示了病毒翻译/复制复合物中存在多种宿主翻译调节因子。耗尽宿主翻译因子如eIF4A2、eIF3A和RACK1会显著降低病毒复制,而耗尽eIF2AK4则没有效果。这些发现突出了病原体操纵宿主机制以自身利益为目的的巧妙之处,清楚地了解这一点对于确定战略靶点和开发针对HEV的特异性抗病毒药物至关重要。戊型肝炎病毒(HEV)是一种通过粪-口途径传播的病原体。由于缺乏有效的实验室模型,该病毒的生命周期了解甚少。在感染过程中,病毒蛋白与宿主蛋白之间的相互作用起着至关重要的作用,清楚地了解这一点对于解读病毒的生命周期至关重要。在本研究中,我们鉴定了所有HEV蛋白的直接宿主相互作用伙伴,并生成了一个PPI网络。我们对HEV-人类PPI网络的功能分析揭示了HEV蛋白在调节多种宿主生物学过程中的作用,如应激和免疫反应、泛素-蛋白酶体系统、能量和铁代谢以及蛋白质翻译。进一步的研究揭示了几种宿主因子在HEV复制中的重要作用。总的来说,我们的研究结果提供了来自HEV及其人类宿主的大量PPI数据资源,并鉴定了病毒翻译/复制机制的分子成分。
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