Literature DB >> 26405031

Hepatitis B Virus Core Protein Phosphorylation Sites Affect Capsid Stability and Transient Exposure of the C-terminal Domain.

Lisa Selzer1, Ravi Kant2, Joseph C-Y Wang1, Brian Bothner2, Adam Zlotnick3.   

Abstract

Hepatitis B virus core protein has 183 amino acids divided into an assembly domain and an arginine-rich C-terminal domain (CTD) that regulates essential functions including genome packaging, reverse transcription, and intracellular trafficking. Here, we investigated the CTD in empty hepatitis B virus (HBV) T=4 capsids. We examined wild-type core protein (Cp183-WT) and a mutant core protein (Cp183-EEE), in which three CTD serines are replaced with glutamate to mimic phosphorylated protein. We found that Cp183-WT capsids were less stable than Cp183-EEE capsids. When we tested CTD sensitivity to trypsin, we detected two different populations of CTDs differentiated by their rate of trypsin cleavage. Interestingly, CTDs from Cp183-EEE capsids exhibited a much slower rate of proteolytic cleavage when compared with CTDs of Cp183-WT capsids. Cryo-electron microscopy studies of trypsin-digested capsids show that CTDs at five-fold symmetry vertices are most protected. We hypothesize that electrostatic interactions between glutamates and arginines in Cp183-EEE, particularly at five-fold, increase capsid stability and reduce CTD exposure. Our studies show that quasi-equivalent CTDs exhibit different rates of exposure and thus might perform distinct functions during the hepatitis B virus lifecycle. Our results demonstrate a structural role for CTD phosphorylation and indicate crosstalk between CTDs within a capsid particle.
© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  capsid stability; cryo-electron microscopy; hepatitis B virus (HBV, Hep B); limited proteolysis; mass spectrometry (MS); phosphorylation; protein dynamics

Mesh:

Substances:

Year:  2015        PMID: 26405031      PMCID: PMC4653712          DOI: 10.1074/jbc.M115.678441

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  37 in total

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10.  Phosphorylation-dependent binding of hepatitis B virus core particles to the nuclear pore complex.

Authors:  M Kann; B Sodeik; A Vlachou; W H Gerlich; A Helenius
Journal:  J Cell Biol       Date:  1999-04-05       Impact factor: 10.539

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  38 in total

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2.  Dynamics of Hepatitis B Virus Capsid Protein Dimer Regulate Assembly through an Allosteric Network.

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Review 3.  The Structural Biology of Hepatitis B Virus: Form and Function.

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Journal:  Annu Rev Virol       Date:  2016-08-01       Impact factor: 10.431

4.  Novel Hepatitis B Virus Capsid-Targeting Antiviral That Aggregates Core Particles and Inhibits Nuclear Entry of Viral Cores.

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Journal:  ACS Infect Dis       Date:  2019-01-14       Impact factor: 5.084

5.  Hepatitis B Virus Core Protein Dephosphorylation Occurs during Pregenomic RNA Encapsidation.

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Journal:  J Virol       Date:  2018-06-13       Impact factor: 5.103

6.  Nanofluidic Devices with 8 Pores in Series for Real-Time, Resistive-Pulse Analysis of Hepatitis B Virus Capsid Assembly.

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7.  A molecular breadboard: Removal and replacement of subunits in a hepatitis B virus capsid.

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8.  Discovery and Mechanistic Study of Benzamide Derivatives That Modulate Hepatitis B Virus Capsid Assembly.

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Review 9.  Targeting the multifunctional HBV core protein as a potential cure for chronic hepatitis B.

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Journal:  Antiviral Res       Date:  2020-08-17       Impact factor: 5.970

10.  Cell-Free Hepatitis B Virus Capsid Assembly Dependent on the Core Protein C-Terminal Domain and Regulated by Phosphorylation.

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Journal:  J Virol       Date:  2016-05-27       Impact factor: 5.103

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