Literature DB >> 24807709

Maintenance of dimer conformation by the dengue virus core protein α4-α4' helix pair is critical for nucleocapsid formation and virus production.

Pak-Guan Teoh1, Zhi-Shun Huang2, Wen-Li Pong2, Po-Chiang Chen2, Huey-Nan Wu3.   

Abstract

The virion of dengue virus (DENV) is composed of a viral envelope covering a nucleocapsid formed by a complex of viral genomic RNA and core protein (CP). DENV CP forms a dimer via the internal α2 and α4 helices of each monomer. Pairing of α2-α2' creates a continuous hydrophobic surface, while the α4-α4' helix pair joins the homodimer via side-chain interactions of the inner-edge residues. However, the importance of dimer conformation and the α4 helix of DENV CP in relation to its function are poorly understood. Loss of association between CP and lipid droplets (LDs) due to mutation suggests that the CP hydrophobic surface was not exposed, offering a possible explanation for the absence of dimers. Further assays suggest the connection between CP folding and protein stability. Attenuation of full-length RNA-derived virus production is associated with CP mutation, since no significant defects were detected in virus translation and replication. The in vitro characterization assays further highlighted that the α4-α4' helix pair conformation is critical in preserving the overall α-helical content, thermostability, and dimer formation ability of CP, features correlated with the efficiency of nucleocapsid formation. Addition of Tween 20 improves in vitro nucleocapsid-like particle formation, suggesting the role of the LD in nucleocapsid formation in vivo. This study provides the first direct link between the α4-α4' helix pair interaction and the CP dimer conformation that is the basis of CP function, particularly in nucleocapsid formation during virion production. Importance: Structure-based mutagenesis study of the dengue virus core protein (CP) reveals that the α4-α4' helix pair is the key to maintaining its dimer conformation, which is the basis of CP function in nucleocapsid formation and virus production. Attenuation of full-length RNA-derived virus production is associated with CP mutation, since no significant defects in virus translation and replication were detected. In vitro inefficiency and size of nucleocapsid-like particle (NLP) formation offer a possible explanation for in vivo virus production inefficiency upon CP mutation. Further, the transition of NLP morphology from an incomplete state to an intact particle shown by α4-α4' helix pair mutants in the presence of a nonionic detergent suggests the regulatory role of the intracellular lipid droplet (LD) in CP-LD interaction and in promoting nucleocapsid formation. This study provides the first direct link between the α4-α4' helix pair interaction and CP dimer conformation that is the fundamental requirement of CP function, particularly in nucleocapsid formation during virion production.
Copyright © 2014, American Society for Microbiology. All Rights Reserved.

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Year:  2014        PMID: 24807709      PMCID: PMC4097798          DOI: 10.1128/JVI.00940-14

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  36 in total

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2.  Intracellular localization and determination of a nuclear localization signal of the core protein of dengue virus.

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3.  Visualization of membrane protein domains by cryo-electron microscopy of dengue virus.

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4.  Flavivirus capsid is a dimeric alpha-helical protein.

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8.  Isolation of capsid protein dimers from the tick-borne encephalitis flavivirus and in vitro assembly of capsid-like particles.

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9.  Solution structure of dengue virus capsid protein reveals another fold.

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  19 in total

1.  Mutation of Putative N-Glycosylation Sites on Dengue Virus NS4B Decreases RNA Replication.

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2.  Zika Virus Dependence on Host Hsp70 Provides a Protective Strategy against Infection and Disease.

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3.  Yellow fever virus capsid protein is a potent suppressor of RNA silencing that binds double-stranded RNA.

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4.  Functional Analysis of the Dengue Virus Genome Using an Insertional Mutagenesis Screen.

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6.  Functional Correlation between Subcellular Localizations of Japanese Encephalitis Virus Capsid Protein and Virus Production.

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7.  Development and characterization of an inducible assay system to measure Zika virus capsid interactions.

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Review 8.  Properties and Functions of the Dengue Virus Capsid Protein.

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Review 9.  Targeting host lipid synthesis and metabolism to inhibit dengue and hepatitis C viruses.

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Review 10.  Structure and function of capsid protein in flavivirus infection and its applications in the development of vaccines and therapeutics.

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