Your search keyword '"Hepatitis B virus chemistry"' showing total 33 results

1. Design, synthesis and evaluation of heteroaryldihydropyrimidine analogues bearing spiro ring as hepatitis B virus capsid protein inhibitors.

Author

Ma Y, Zhao S, Ren Y, Cherukupalli S, Li Q, Woodson ME, Bradley DP, Tavis JE, Liu X, and Zhan P

Subjects

Antiviral Agents chemical synthesis, Antiviral Agents chemistry, Capsid Proteins metabolism, Dose-Response Relationship, Drug, Hepatitis B virus chemistry, Hepatitis B virus metabolism, Humans, Microbial Sensitivity Tests, Molecular Structure, Pyrimidines chemical synthesis, Pyrimidines chemistry, Structure-Activity Relationship, Antiviral Agents pharmacology, Capsid Proteins antagonists & inhibitors, Drug Design, Hepatitis B virus drug effects, Pyrimidines pharmacology

Abstract

GLS4, a potent antiviral drug candidate, has been widely studied and entered into phase II clinical trials. Nevertheless, the therapeutic application of GLS4 is limited due to poor water solubility, short half-life, and low bioavailability. In order to improve the hydrophilicity and pharmacokinetic (PK) properties of GLS4, herein, we retained the dominant fragments, and used a scaffold hopping strategy to replace the easily metabolized morpholine ring of GLS4 with diverse sizes of spiro rings consisting of hydrogen bond donor and acceptor substituents. Potent in vitroanti-HBV activity and low cytotoxicity were observed for compound 4r (EC 50  = 0.20 ± 0.00 μM, CC 50  > 87.03 μM), which was more potent than the positive control lamivudine (EC 50  = 0.37 ± 0.04 μM, CC 50  > 100.00 μM) in this assay and was about a quarter as effective as GLS4 (EC 50  = 0.045 ± 0.01 μM, CC 50  > 99.20 μM). Preliminary structure-activity relationship (SAR) analysis and molecular docking studies were carried out to explore potential interactions and binding mode between compounds and target protein. In terms of the physicochemical properties, 4r was predicted to be consistent with the rule-of-five, which means 4r may have favourable absorption and permeation. Finally, ADMET and PK characteristics of 4r and GLS4 were predicted to be comparable in most aspects, implying that the two compounds may have similar profiles in vivo., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper. The authors declare no conflict of interest., (Copyright © 2021 Elsevier Masson SAS. All rights reserved.)

Published

2021

2. A pocket-factor-triggered conformational switch in the hepatitis B virus capsid.

Author

Lecoq L, Wang S, Dujardin M, Zimmermann P, Schuster L, Fogeron ML, Briday M, Schledorn M, Wiegand T, Cole L, Montserret R, Bressanelli S, Meier BH, Nassal M, and Böckmann A

Subjects

Protein Conformation, Capsid Proteins chemistry, Hepatitis B virus chemistry

Abstract

Viral hepatitis is growing into an epidemic illness, and it is urgent to neutralize the main culprit, hepatitis B virus (HBV), a small-enveloped retrotranscribing DNA virus. An intriguing observation in HB virion morphogenesis is that capsids with immature genomes are rarely enveloped and secreted. This prompted, in 1982, the postulate that a regulated conformation switch in the capsid triggers envelopment. Using solid-state NMR, we identified a stable alternative conformation of the capsid. The structural variations focus on the hydrophobic pocket of the core protein, a hot spot in capsid-envelope interactions. This structural switch is triggered by specific, high-affinity binding of a pocket factor. The conformational change induced by the binding is reminiscent of a maturation signal. This leads us to formulate the "synergistic double interaction" hypothesis, which explains the regulation of capsid envelopment and indicates a concept for therapeutic interference with HBV envelopment., Competing Interests: The authors declare no competing interest., (Copyright © 2021 the Author(s). Published by PNAS.)

Published

2021

3. All-Atom MD Simulations of the HBV Capsid Complexed with AT130 Reveal Secondary and Tertiary Structural Changes and Mechanisms of Allostery.

Author

Pérez-Segura C, Goh BC, and Hadden-Perilla JA

Subjects

Allosteric Site, Antiviral Agents pharmacology, Benzamides pharmacology, Capsid drug effects, Capsid metabolism, Computational Biology methods, Hepatitis B virus drug effects, Hepatitis B virus genetics, Humans, Protein Multimerization, Virus Assembly, Benzamides metabolism, Capsid chemistry, Capsid Proteins metabolism, Hepatitis B virus chemistry, Molecular Dynamics Simulation

Abstract

The hepatitis B virus (HBV) capsid is an attractive drug target, relevant to combating viral hepatitis as a major public health concern. Among small molecules known to interfere with capsid assembly, the phenylpropenamides, including AT130, represent an important antiviral paradigm based on disrupting the timing of genome packaging. Here, all-atom molecular dynamics simulations of an intact AT130-bound HBV capsid reveal that the compound increases spike flexibility and improves recovery of helical secondary structure in the spike tips. Regions of the capsid-incorporated dimer that undergo correlated motion correspond to established sub-domains that pivot around the central chassis. AT130 alters patterns of correlated motion and other essential dynamics. A new conformational state of the dimer is identified, which can lead to dramatic opening of the intradimer interface and disruption of communication within the spike tip. A novel salt bridge is also discovered, which can mediate contact between the spike tip and fulcrum even in closed conformations, revealing a mechanism of direct communication across these sub-domains. Altogether, results describe a dynamical connection between the intra- and interdimer interfaces and enable mapping of allostery traversing the entire core protein dimer.

Published

2021

4. The Integrity of the Intradimer Interface of the Hepatitis B Virus Capsid Protein Dimer Regulates Capsid Self-Assembly.

Author

Zhao Z, Wang JC, Segura CP, Hadden-Perilla JA, and Zlotnick A

Subjects

Dimerization, Hepatitis B virus physiology, Molecular Dynamics Simulation, Protein Conformation, Reproducibility of Results, Capsid chemistry, Capsid Proteins chemistry, Hepatitis B virus chemistry

Abstract

During the hepatitis B virus lifecycle, 120 copies of homodimeric capsid protein assemble around a copy of reverse transcriptase and viral RNA and go on to produce an infectious virion. Assembly needs to be tightly regulated by protein conformational change to ensure symmetry, fidelity, and reproducibility. Here, we show that structures at the intradimer interface regulate conformational changes at the distal interdimer interface and so regulate assembly. A pair of interacting charged residues, D78 from each monomer, conspicuously located at the top of a four-helix bundle that forms the intradimer interface, were mutated to serine to disrupt communication between the two monomers. The mutation slowed assembly and destabilized the dimer to thermal and chemical denaturation. Mutant dimers showed evidence of transient partial unfolding based on the appearance of new proteolytically sensitive sites. Though the mutant dimer was less stable, the resulting capsids were as stable as the wildtype, based on assembly and thermal denaturation studies. Cryo-EM image reconstructions of capsid indicated that the subunits adopted an "open" state more usually associated with a free dimer and that the spike tips were either disordered or highly flexible. Molecular dynamics simulations provide mechanistic explanations for these results, suggesting that D78 stabilizes helix 4a, which forms part of the intradimer interface, by capping its N-terminus and hydrogen-bonding to nearby residues, whereas the D78S mutation disrupts these interactions, leading to partial unwinding of helix 4a. This in turn weakens the connection from helix 4 and the intradimer interface to helix 5, which forms the interdimer interface.

Published

2020

5. Higher Resolution Charge Detection Mass Spectrometry.

Author

Todd AR, Barnes LF, Young K, Zlotnick A, and Jarrold MF

Subjects

Capsid metabolism, Hepatitis B virus chemistry, Hepatitis B virus metabolism, Capsid chemistry, Capsid Proteins analysis, Mass Spectrometry methods

Abstract

Charge detection mass spectrometry is a single particle technique where the masses of individual ions are determined from simultaneous measurements of each ion's m / z ratio and charge. The ions pass through a conducting cylinder, and the charge induced on the cylinder is detected. The cylinder is usually placed inside an electrostatic linear ion trap so that the ions oscillate back and forth through the cylinder. The resulting time domain signal is analyzed by fast Fourier transformation; the oscillation frequency yields the m / z , and the charge is determined from the magnitudes. The mass resolving power depends on the uncertainties in both quantities. In previous work, the mass resolving power was modest, around 30-40. In this work we report around an order of magnitude improvement. The improvement was achieved by coupling high-accuracy charge measurements (obtained with dynamic calibration) with higher resolution m / z measurements. The performance was benchmarked by monitoring the assembly of the hepatitis B virus (HBV) capsid. The HBV capsid assembly reaction can result in a heterogeneous mixture of intermediates extending from the capsid protein dimer to the icosahedral T = 4 capsid with 120 dimers. Intermediates of all possible sizes were resolved, as well as some overgrown species. Despite the improved mass resolving power, the measured peak widths are still dominated by instrumental resolution. Heterogeneity makes only a small contribution. Resonances were observed in some of the m / z spectra. They result from ions with different masses and charges having similar m / z values. Analogous resonances are expected whenever the sample is a heterogeneous mixture assembled from a common building block.

Published

2020

6. Expression of quasi-equivalence and capsid dimorphism in the Hepadnaviridae.

Author

Wu W, Watts NR, Cheng N, Huang R, Steven AC, and Wingfield PT

Subjects

Amino Acid Sequence, Binding Sites, Computational Biology methods, Protein Conformation, Protein Multimerization, Thermodynamics, Capsid chemistry, Capsid metabolism, Capsid Proteins chemistry, Capsid Proteins metabolism, Hepatitis B virus chemistry, Protein Subunits chemistry, Protein Subunits metabolism

Abstract

Hepatitis B virus (HBV) is a leading cause of liver disease. The capsid is an essential component of the virion and it is therefore of interest how it assembles and disassembles. The capsid protein is unusual both for its rare fold and that it polymerizes according to two different icosahedral symmetries, causing the polypeptide chain to exist in seven quasi-equivalent environments: A, B, and C in AB and CC dimers in T = 3 capsids, and A, B, C, and D in AB and CD dimers in T = 4 capsids. We have compared the two capsids by cryo-EM at 3.5 Å resolution. To ensure a valid comparison, the two capsids were prepared and imaged under identical conditions. We find that the chains have different conformations and potential energies, with the T = 3 C chain having the lowest. Three of the four quasi-equivalent dimers are asymmetric with respect to conformation and potential energy; however, the T = 3 CC dimer is symmetrical and has the lowest potential energy although its intra-dimer interface has the least free energy of formation. Of all the inter-dimer interfaces, the CB interface has the least area and free energy, in both capsids. From the calculated energies of higher-order groupings of dimers discernible in the lattices we predict early assembly intermediates, and indeed we observe such structures by negative stain EM of in vitro assembly reactions. By sequence analysis and computational alanine scanning we identify key residues and motifs involved in capsid assembly. Our results explain several previously reported observations on capsid assembly, disassembly, and dimorphism., Competing Interests: The authors have declared that no competing interests exist.

Published

2020

7. Dramatic Improvement in Sensitivity with Pulsed Mode Charge Detection Mass Spectrometry.

Author

Todd AR and Jarrold MF

Subjects

Mass Spectrometry, Static Electricity, Capsid Proteins analysis, Hepatitis B virus chemistry

Abstract

Charge detection mass spectrometry (CDMS) is emerging as a valuable tool to determine mass distributions for heterogeneous and high-mass samples. It is a single-particle technique where masses are determined for individual ions from simultaneous measurements of their mass-to-charge ratio ( m / z ) and charge. Ions are trapped in an electrostatic linear ion trap (ELIT) and oscillate back and forth through a detection cylinder. The trap is open and able to trap ions for a small fraction of the total measurement time so most of the ions (>99.8%) in a continuous ion beam are lost. Here, we implement an ion storage scheme where ions are accumulated and stored in a hexapole and then injected into the ELIT at the right time for them to be trapped. This pulsed mode of operation increases the sensitivity of CDMS by more than 2 orders of magnitude, which allows much lower titer samples to be analyzed. A limit of detection of 3.3 × 10 8 particles/mL was obtained for hepatitis B virus T = 4 capsids with a 1.3 μL sample. The hexapole where the ions are accumulated and stored is a significant distance from the ion trap so ions are dispersed in time by their m / z values as they travel between the hexapole and the ELIT. By varying the delay time between ion release and trapping, different windows of m / z values can be trapped.

Published

2019

8. Assembly Reactions of Hepatitis B Capsid Protein into Capsid Nanoparticles Follow a Narrow Path through a Complex Reaction Landscape.

Author

Asor R, Selzer L, Schlicksup CJ, Zhao Z, Zlotnick A, and Raviv U

Subjects

Capsid Proteins isolation & purification, Entropy, Molecular Dynamics Simulation, Monte Carlo Method, Capsid chemistry, Capsid Proteins chemistry, Hepatitis B virus chemistry, Nanoparticles chemistry

Abstract

For many viruses, capsids (biological nanoparticles) assemble to protect genetic material and dissociate to release their cargo. To understand these contradictory properties, we analyzed capsid assembly for hepatitis B virus; an endemic pathogen with an icosahedral, 120-homodimer capsid. We used solution X-ray scattering to examine trapped and equilibrated assembly reactions. To fit experimental results, we generated a library of distinct intermediates, selected by umbrella sampling of Monte Carlo simulations. The number of possible capsid intermediates is immense, ∼10 30 , yet assembly reactions are rapid and completed with high fidelity. If the huge number of possible intermediates were actually present, maximum entropy analysis shows that assembly reactions would be blocked by an entropic barrier, resulting in incomplete nanoparticles. When an energetic term was applied to select the stable species that dominated the reaction mixture, we found only a few hundred intermediates, mapping out a narrow path through the immense reaction landscape. This is a solution to a viral application of the Levinthal paradox. With the correct energetic term, the match between predicted intermediates and scattering data was striking. The grand canonical free energy landscape for assembly, calibrated by our experimental results, supports a detailed analysis of this complex reaction. There is a narrow range of energies that supports on-path assembly. If association energy is too weak or too strong, progressively more intermediates will be entropically blocked, spilling into paths leading to dissociation or trapped incomplete nanoparticles, respectively. These results are relevant to many viruses and provide a basis for simplifying assembly models and identifying new targets for antiviral intervention. They provide a basis for understanding and designing biological and abiological self-assembly reactions.

Published

2019

9. An Assembly-Activating Site in the Hepatitis B Virus Capsid Protein Can Also Trigger Disassembly.

Author

Qazi S, Schlicksup CJ, Rittichier J, VanNieuwenhze MS, and Zlotnick A

Subjects

Capsid Proteins chemistry, Hepatitis B virus chemistry, Humans, Models, Molecular, Protein Multimerization, Capsid Proteins metabolism, Hepatitis B virology, Hepatitis B virus physiology, Virus Assembly

Abstract

The Hepatitis B Virus (HBV) core protein homodimers self-assemble to form an icosahedral capsid that packages the viral genome. Disassembly occurs in the nuclear basket to release the mature genome to the nucleus. Small molecules have been developed that bind to a pocket at the interdimer interface to accelerate assembly and strengthen interactions between subunits; these are under development as antiviral agents. Here, we explore the role of the dimer-dimer interface by mutating sites in the drug-binding pocket to cysteine and examining the effect of covalently linking small molecules to them. We find that ligands bound to the pocket may trigger capsid disassembly in a dose-dependent manner. This result indicates that, at least transiently, the pocket adopts a destabilizing conformation. We speculate that this pocket also plays a role in virus disassembly and genome release by binding ligands that are incompatible with virus stability, "unwanted guests." Investigating protein-protein interactions, especially large protein polymers, offers new and unique challenges. By using an engineered addressable thiol, we provide a means to examine the effects of modifying an interface without requiring drug-like properties for the ligand.

Published

2018

10. Identification of Factors Promoting HBV Capsid Self-Assembly by Assembly-Promoting Antivirals.

Author

Rath SL, Liu H, Okazaki S, and Shinoda W

Subjects

Allosteric Regulation, Dimerization, Drug Delivery Systems, Drug Design, Genome, Viral, Hepatitis B virus chemistry, Hepatitis B virus genetics, Molecular Dynamics Simulation, Protein Binding, Protein Domains, Antiviral Agents pharmacology, Capsid Proteins chemistry, Hepatitis B virus physiology, Virus Assembly

Abstract

Around 270 million individuals currently live with hepatitis B virus (HBV) infection. Heteroaryldihydropyrimidines (HAPs) are a family of antivirals that target the HBV capsid protein and induce aberrant self-assembly. The capsids formed resemble the native capsid structure but are unable to propagate the virus progeny because of a lack of RNA/DNA. Under normal conditions, self-assembly is initiated by the viral genome. The mode of action of HAPs, however, remains largely unknown. In this work, using molecular dynamics simulations, we attempted to understand the action of HAP by comparing the dynamics of capsid proteins with and without HAPs. We found that the inhibitor is more stable in higher oligomers. It retains its stability in the hexamer throughout 1 μs of simulation. Our results also show that the inhibitor might help in stabilizing the C-terminus, the HBc 149-183 arginine-rich domain of the capsid protein. The C-termini of dimers interact with each other, assisted by the HAP inhibitor. During capsid assembly, the termini are supposed to directly interact with the viral genome, thereby suggesting that the viral genome might work in a similar way to stabilize the capsid protein. Our results may help in understanding the underlying molecular mechanism of HBV capsid self-assembly, which should be crucial for exploring new drug targets and structure-based drug design.

Published

2018

11. Displaying Whole-Chain Proteins on Hepatitis B Virus Capsid-Like Particles.

Author

Heger-Stevic J, Kolb P, Walker A, and Nassal M

Subjects

Borrelia burgdorferi genetics, Borrelia burgdorferi pathogenicity, Epitopes genetics, Epitopes immunology, Escherichia coli genetics, Hepatitis B Core Antigens chemistry, Hepatitis B Core Antigens immunology, Hepatitis B virus genetics, Hepatitis B virus immunology, Nanoparticles chemistry, Capsid Proteins chemistry, Hepatitis B Core Antigens genetics, Hepatitis B virus chemistry

Abstract

The highly immunogenic icosahedral capsid of hepatitis B virus (HBV) can be exploited as a nanoparticulate display platform for heterologous molecules. Its constituent core protein (HBc) of only ~180 amino acids spontaneously forms capsid-like particles (CLPs) even in E. coli. The immunodominant c/e1 epitope in the center of the HBc primary sequence comprises a solvent-exposed loop that tolerates insertions of flexible peptide sequences yet also of selected whole proteins as long as their 3D structures fit into the two acceptor sites. This constraint is largely overcome in the SplitCore system, where the sequences flanking the loop are expressed as two separate but self-complementing entities, with the foreign sequence fixed to the carrier at one end only. Both the contiguous and the split type of CLP strongly enhance immunogenicity of the displayed sequence but also nonvaccine applications can easily be envisaged. After a brief survey of the basic features of the two HBc carrier forms, we provide conceptual guidelines concerning which foreign proteins are likely to be presentable, or not, on either carrier type. We describe generally applicable protocols for CLP expression in E. coli, cell lysis and CLP enrichment by sucrose gradient velocity sedimentation, plus a simple but meaningful gel electrophoretic assay to assess proper particle formation.

Published

2018

12. Kinetics versus Thermodynamics in Virus Capsid Polymorphism.

Author

Moerman P, van der Schoot P, and Kegel W

Subjects

Capsid ultrastructure, Capsid Proteins ultrastructure, Hepatitis B virus ultrastructure, Kinetics, Thermodynamics, Virion ultrastructure, Virus Assembly physiology, Capsid chemistry, Capsid Proteins chemistry, Hepatitis B virus chemistry, Virion chemistry

Abstract

Virus coat proteins spontaneously self-assemble into empty shells in aqueous solution under the appropriate physicochemical conditions, driven by an interaction free energy per bond on the order of 2-5 times the thermal energy kBT. For this seemingly modest interaction strength, each protein building block nonetheless gains a very large binding free energy, between 10 and 20 kBT. Because of this, there is debate about whether the assembly process is reversible or irreversible. Here we discuss capsid polymorphism observed in in vitro experiments from the perspective of nucleation theory and of the thermodynamics of mass action. We specifically consider the potential contribution of a curvature free energy term to the effective interaction potential between the proteins. From these models, we propose experiments that may conclusively reveal whether virus capsid assembly into a mixture of polymorphs is a reversible or an irreversible process.

Published

2016

13. Hepatitis B Virus Capsids Have Diverse Structural Responses to Small-Molecule Ligands Bound to the Heteroaryldihydropyrimidine Pocket.

Author

Venkatakrishnan B, Katen SP, Francis S, Chirapu S, Finn MG, and Zlotnick A

Subjects

Allosteric Site, Antiviral Agents chemistry, Capsid metabolism, Capsid Proteins metabolism, Crystallography, Hepatitis B Core Antigens chemistry, Hepatitis B Core Antigens metabolism, Hepatitis B virus metabolism, Models, Molecular, Protein Binding, Protein Conformation, Pyrimidines metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Viral Core Proteins chemistry, Viral Core Proteins metabolism, Capsid chemistry, Capsid Proteins chemistry, Hepatitis B virus chemistry, Pyrimidines chemistry

Abstract

Unlabelled: Though the hepatitis B virus (HBV) core protein is an important participant in many aspects of the viral life cycle, its best-characterized activity is self-assembly into 240-monomer capsids. Small molecules that target core protein (core protein allosteric modulators [CpAMs]) represent a promising antiviral strategy. To better understand the structural basis of the CpAM mechanism, we determined the crystal structure of the HBV capsid in complex with HAP18. HAP18 accelerates assembly, increases protein-protein association more than 100-fold, and induces assembly of nonicosahedral macrostructures. In a preformed capsid, HAP18 is found at quasiequivalent subunit-subunit interfaces. In a detailed comparison to the two other extant CpAM structures, we find that the HAP18-capsid structure presents a paradox. Whereas the two other structures expanded the capsid diameter by up to 10 Å, HAP18 caused only minor changes in quaternary structure and actually decreased the capsid diameter by ∼3 Å. These results indicate that CpAMs do not have a single allosteric effect on capsid structure. We suggest that HBV capsids present an ensemble of states that can be trapped by CpAMs, indicating a more complex basis for antiviral drug design., Importance: Hepatitis B virus core protein has multiple roles in the viral life cycle-assembly, compartment for reverse transcription, intracellular trafficking, and nuclear functions-making it an attractive antiviral target. Core protein allosteric modulators (CpAMs) are an experimental class of antivirals that bind core protein. The most recognized CpAM activity is that they accelerate core protein assembly and strengthen interactions between subunits. In this study, we observe that the CpAM-binding pocket has multiple conformations. We compare structures of capsids cocrystallized with different CpAMs and find that they also affect quaternary structure in different ways. These results suggest that the capsid "breathes" and is trapped in different states by the drug and crystallization. Understanding that the capsid is a moving target will aid drug design and improve our understanding of HBV interaction with its environment., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2016

14. Tabulation as a high-resolution alternative to coarse-graining protein interactions: Initial application to virus capsid subunits.

Author

Spiriti J and Zuckerman DM

Subjects

Monte Carlo Method, Capsid chemistry, Capsid Proteins chemistry, Hepatitis B virus chemistry, Molecular Dynamics Simulation, Protein Subunits chemistry

Abstract

Traditional coarse-graining based on a reduced number of interaction sites often entails a significant sacrifice of chemical accuracy. As an alternative, we present a method for simulating large systems composed of interacting macromolecules using an energy tabulation strategy previously devised for small rigid molecules or molecular fragments [S. Lettieri and D. M. Zuckerman, J. Comput. Chem. 33, 268-275 (2012); J. Spiriti and D. M. Zuckerman, J. Chem. Theory Comput. 10, 5161-5177 (2014)]. We treat proteins as rigid and construct distance and orientation-dependent tables of the interaction energy between them. Arbitrarily detailed interactions may be incorporated into the tables, but as a proof-of-principle, we tabulate a simple α-carbon Gō-like model for interactions between dimeric subunits of the hepatitis B viral capsid. This model is significantly more structurally realistic than previous models used in capsid assembly studies. We are able to increase the speed of Monte Carlo simulations by a factor of up to 6700 compared to simulations without tables, with only minimal further loss in accuracy. To obtain further enhancement of sampling, we combine tabulation with the weighted ensemble (WE) method, in which multiple parallel simulations are occasionally replicated or pruned in order to sample targeted regions of a reaction coordinate space. In the initial study reported here, WE is able to yield pathways of the final ∼25% of the assembly process.

Published

2015

15. Monitoring Assembly of Virus Capsids with Nanofluidic Devices.

Author

Harms ZD, Selzer L, Zlotnick A, and Jacobson SC

Subjects

Capsid chemistry, Capsid metabolism, Capsid Proteins metabolism, Hepatitis B virus metabolism, Kinetics, Protein Multimerization, Virion chemistry, Virion metabolism, Capsid Proteins chemistry, Hepatitis B virus chemistry, Virus Assembly

Abstract

Virus assembly is a coordinated process in which typically hundreds of subunits react to form complex, symmetric particles. We use resistive-pulse sensing to characterize the assembly of hepatitis B virus core protein dimers into T = 3 and T = 4 icosahedral capsids. This technique counts and sizes intermediates and capsids in real time, with single-particle sensitivity, and at biologically relevant concentrations. Other methods are not able to produce comparable real-time, single-particle observations of assembly reactions below, near, and above the pseudocritical dimer concentration, at which the dimer and capsid concentrations are approximately equal. Assembly reactions across a range of dimer concentrations reveal three distinct patterns. At dimer concentrations as low as 50 nM, well below the pseudocritical dimer concentration of 0.5 μM, we observe a switch in the ratio of T = 3 to T = 4 capsids, which increases with decreasing dimer concentration. Far above the pseudocritical dimer concentration, kinetically trapped, incomplete T = 4 particles assemble rapidly, then slowly anneal into T = 4 capsids. At all dimer concentrations tested, T = 3 capsids form more rapidly than T = 4 capsids, suggesting distinct pathways for the two forms.

Published

2015

16. Advances in Single-Particle Electron Cryomicroscopy Structure Determination applied to Sub-tomogram Averaging.

Author

Bharat TAM, Russo CJ, Löwe J, Passmore LA, and Scheres SHW

Subjects

Algorithms, Bayes Theorem, Hepatitis B virus chemistry, Imaging, Three-Dimensional methods, Models, Molecular, Protein Conformation, Capsid Proteins chemistry, Cryoelectron Microscopy methods, Hepatitis B virus metabolism

Abstract

Recent innovations in specimen preparation, data collection, and image processing have led to improved structure determination using single-particle electron cryomicroscopy (cryo-EM). Here we explore some of these advances to improve structures determined using electron cryotomography (cryo-ET) and sub-tomogram averaging. We implement a new three-dimensional model for the contrast transfer function, and use this in a regularized likelihood optimization algorithm as implemented in the RELION program. Using direct electron detector data, we apply both single-particle analysis and sub-tomogram averaging to analyze radiation-induced movements of the specimen. As in single-particle cryo-EM, we find that significant sample movements occur during tomographic data acquisition, and that these movements are substantially reduced through the use of ultrastable gold substrates. We obtain a sub-nanometer resolution structure of the hepatitis B capsid, and show that reducing radiation-induced specimen movement may be central to attempts at further improving tomogram quality and resolution., (Copyright © 2015 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2015

17. Assembly Pathway of Hepatitis B Core Virus-like Particles from Genetically Fused Dimers.

Author

Holmes K, Shepherd DA, Ashcroft AE, Whelan M, Rowlands DJ, and Stonehouse NJ

Subjects

Capsid chemistry, Capsid metabolism, Capsid Proteins genetics, Dimerization, Hepatitis B virus chemistry, Hepatitis B virus genetics, Hepatitis B virus ultrastructure, Models, Molecular, Virion chemistry, Virion genetics, Virion ultrastructure, Virus Assembly, Capsid Proteins chemistry, Capsid Proteins metabolism, Hepatitis B virus metabolism, Virion metabolism

Abstract

Macromolecular complexes are responsible for many key biological processes. However, in most cases details of the assembly/disassembly of such complexes are unknown at the molecular level, as the low abundance and transient nature of assembly intermediates make analysis challenging. The assembly of virus capsids is an example of such a process. The hepatitis B virus capsid (core) can be composed of either 90 or 120 dimers of coat protein. Previous studies have proposed a trimer of dimers as an important intermediate species in assembly, acting to nucleate further assembly by dimer addition. Using novel genetically-fused coat protein dimers, we have been able to trap higher-order assembly intermediates and to demonstrate for the first time that both dimeric and trimeric complexes are on pathway to virus-like particle (capsid) formation., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

18. Coat Protein-Dependent Behavior of Poly(ethylene glycol) Tails in Iron Oxide Core Virus-like Nanoparticles.

Author

Malyutin AG, Cheng H, Sanchez-Felix OR, Carlson K, Stein BD, Konarev PV, Svergun DI, Dragnea B, and Bronstein LM

Subjects

Capsid Proteins therapeutic use, Ferric Compounds chemistry, Ferric Compounds therapeutic use, Humans, Hydrophobic and Hydrophilic Interactions, Magnetic Resonance Imaging, Nanoparticles therapeutic use, Polyethylene Glycols chemistry, Polyethylene Glycols therapeutic use, Polymers chemistry, Polymers therapeutic use, Bromovirus chemistry, Capsid Proteins chemistry, Hepatitis B virus chemistry, Nanoparticles chemistry

Abstract

Here we explore the formation of virus-like nanoparticles (VNPs) utilizing 22-24 nm iron oxide nanoparticles (NPs) as cores and proteins derived from viral capsids of brome mosaic virus (BMV) or hepatitis B virus (HBV) as shells. To accomplish that, hydrophobic FeO/Fe3O4 NPs prepared by thermal decomposition of iron oleate were coated with poly(maleic acid-alt-octadecene) modified with poly(ethylene glycol) (PEG) tails of different lengths and grafting densities. MRI studies show high r2/r1 relaxivity ratios of these NPs that are practically independent of the polymer coating type. The versatility and flexibility of the viral capsid protein are on display as they readily form shells that exceed their native size. The location of the long PEG tails upon shell formation was investigated by electron microscopy and small-angle X-ray scattering. PEG tails were located differently in the BMV and HBV VNPs, with the BMV VNPs preferentially entrapping the tails in the interior and the HBV VNPs allowing the tails to extend through the capsid, which highlights the differences between intersubunit interactions in these two icosahedral viruses. The robustness of the assembly reaction and the protruding PEG tails, potentially useful in modulating the immune response, make the systems introduced here a promising platform for biomedical applications.

Published

2015

19. The interface between hepatitis B virus capsid proteins affects self-assembly, pregenomic RNA packaging, and reverse transcription.

Author

Tan Z, Pionek K, Unchwaniwala N, Maguire ML, Loeb DD, and Zlotnick A

Subjects

Capsid chemistry, Capsid Proteins chemistry, Capsid Proteins genetics, Gene Expression Regulation, Viral, Hepatitis B virus chemistry, Hepatitis B virus enzymology, Hepatitis B virus genetics, Humans, Kinetics, Protein Structure, Tertiary, RNA, Viral genetics, RNA-Directed DNA Polymerase genetics, RNA-Directed DNA Polymerase metabolism, Viral Proteins genetics, Viral Proteins metabolism, Capsid metabolism, Capsid Proteins metabolism, Hepatitis B virology, Hepatitis B virus metabolism, RNA, Viral metabolism, Reverse Transcription

Abstract

Unlabelled: Hepatitis B virus (HBV) capsid proteins (Cps) assemble around the pregenomic RNA (pgRNA) and viral reverse transcriptase (P). pgRNA is then reverse transcribed to double-stranded DNA (dsDNA) within the capsid. The Cp assembly domain, which forms the shell of the capsid, regulates assembly kinetics and capsid stability. The Cp, via its nucleic acid-binding C-terminal domain, also affects nucleic acid organization. We hypothesize that the structure of the capsid may also have a direct effect on nucleic acid processing. Using structure-guided design, we made a series of mutations at the interface between Cp subunits that change capsid assembly kinetics and thermodynamics in a predictable manner. Assembly in cell culture mirrored in vitro activity. However, all of these mutations led to defects in pgRNA packaging. The amount of first-strand DNA synthesized was roughly proportional to the amount of RNA packaged. However, the synthesis of second-strand DNA, which requires two template switches, was not supported by any of the substitutions. These data demonstrate that the HBV capsid is far more than an inert container, as mutations in the assembly domain, distant from packaged nucleic acid, affect reverse transcription. We suggest that capsid molecular motion plays a role in regulating genome replication., Importance: The hepatitis B virus (HBV) capsid plays a central role in the virus life cycle and has been studied as a potential antiviral target. The capsid protein (Cp) packages the viral pregenomic RNA (pgRNA) and polymerase to form the HBV core. The role of the capsid in subsequent nucleic acid metabolism is unknown. Here, guided by the structure of the capsid with bound antiviral molecules, we designed Cp mutants that enhanced or attenuated the assembly of purified Cp in vitro. In cell culture, assembly of mutants was consistent with their in vitro biophysical properties. However, all of these mutations inhibited HBV replication. Specifically, changing the biophysical chemistry of Cp caused defects in pgRNA packaging and synthesis of the second strand of DNA. These results suggest that the HBV Cp assembly domain potentially regulates reverse transcription, extending the activities of the capsid protein beyond its presumed role as an inert compartment., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

20. A molecular thermodynamic model for the stability of hepatitis B capsids.

Author

Kim J and Wu J

Subjects

Hepatitis B genetics, Hepatitis B virology, Hepatitis B virus genetics, Hydrophobic and Hydrophilic Interactions, Models, Theoretical, Thermodynamics, Virus Assembly, Capsid Proteins chemistry, Hepatitis B virus chemistry, Molecular Dynamics Simulation, RNA chemistry

Abstract

Self-assembly of capsid proteins and genome encapsidation are two critical steps in the life cycle of most plant and animal viruses. A theoretical description of such processes from a physiochemical perspective may help better understand viral replication and morphogenesis thus provide fresh insights into the experimental studies of antiviral strategies. In this work, we propose a molecular thermodynamic model for predicting the stability of Hepatitis B virus (HBV) capsids either with or without loading nucleic materials. With the key components represented by coarse-grained thermodynamic models, the theoretical predictions are in excellent agreement with experimental data for the formation free energies of empty T4 capsids over a broad range of temperature and ion concentrations. The theoretical model predicts T3/T4 dimorphism also in good agreement with the capsid formation at in vivo and in vitro conditions. In addition, we have studied the stability of the viral particles in response to physiological cellular conditions with the explicit consideration of the hydrophobic association of capsid subunits, electrostatic interactions, molecular excluded volume effects, entropy of mixing, and conformational changes of the biomolecular species. The course-grained model captures the essential features of the HBV nucleocapsid stability revealed by recent experiments.

Published

2014

21. Phase diagrams map the properties of antiviral agents directed against hepatitis B virus core assembly.

Author

Li L, Chirapu SR, Finn MG, and Zlotnick A

Subjects

Binding Sites, Kinetics, Models, Molecular, Protein Binding, Protein Multimerization, Thermodynamics, Viral Core Proteins antagonists & inhibitors, Virus Assembly, Antiviral Agents chemistry, Benzamides chemistry, Capsid chemistry, Capsid Proteins chemistry, Hepatitis B virus chemistry, Pyrimidines chemistry, Viral Core Proteins chemistry

Abstract

Assembly effectors are small molecules that induce inappropriate virus capsid assembly to antiviral effect. To identify attributes of hepatitis B virus (HBV) assembly effectors, assembly reaction products (normal capsid, noncapsid polymer, intermediates, and free dimeric core protein) were quantified in the presence of three experimental effectors: HAP12, HAP13, and AT-130. Effectors bound stoichiometrically to capsid protein polymers, but not free protein. Thermodynamic and kinetic effects, not aberrant assembly, correlate with maximal antiviral activity.

Published

2013

22. Structural organization of pregenomic RNA and the carboxy-terminal domain of the capsid protein of hepatitis B virus.

Author

Wang JC, Dhason MS, and Zlotnick A

Subjects

Capsid metabolism, DNA, Viral genetics, DNA, Viral metabolism, Genome, Viral, Hepatitis B virus ultrastructure, Molecular Chaperones, Phosphorylation, Protein Structure, Tertiary, RNA, Viral genetics, Capsid ultrastructure, Capsid Proteins chemistry, Capsid Proteins metabolism, Hepatitis B virus chemistry, Hepatitis B virus genetics, RNA, Viral metabolism, Virus Assembly

Abstract

The Hepatitis B Virus (HBV) double-stranded DNA genome is reverse transcribed from its RNA pregenome (pgRNA) within the virus core (or capsid). Phosphorylation of the arginine-rich carboxy-terminal domain (CTD) of the HBV capsid protein (Cp183) is essential for pgRNA encapsidation and reverse transcription. However, the structure of the CTD remains poorly defined. Here we report sub-nanometer resolution cryo-EM structures of in vitro assembled empty and pgRNA-filled Cp183 capsids in unphosphorylated and phosphorylation-mimic states. In empty capsids, we found unexpected evidence of surface accessible CTD density partially occluding pores in the capsid surface. We also observed that CTD organization changed substantively as a function of phosphorylation. In RNA-filled capsids, unphosphorylated CTDs favored thick ropes of RNA, while the phosphorylation-mimic favored a mesh of thin, high-density strands suggestive of single stranded RNA. These results demonstrate that the CTD can regulate nucleic acid structure, supporting the hypothesis that the HBV capsid has a functional role as a nucleic acid chaperone.

Published

2012

23. Cryo-EM study of Hepatitis B virus core antigen capsids decorated with antibodies from a human patient.

Author

Kandiah E, Watts NR, Cheng N, Cardone G, Stahl SJ, Heller T, Liang TJ, Wingfield PT, and Steven AC

Subjects

Animals, Antibodies, Monoclonal chemistry, Antibodies, Monoclonal immunology, Epitopes immunology, Hepatitis Antibodies immunology, Humans, Image Processing, Computer-Assisted, Mice, Protein Structure, Tertiary, Capsid Proteins chemistry, Cryoelectron Microscopy methods, Epitopes chemistry, Hepatitis Antibodies chemistry, Hepatitis B virus chemistry

Abstract

The capsid (core antigen, HBcAg) is one of three major antigens present in patients infected with Hepatitis B virus. The capsids are icosahedral particles, whose most prominent features are spikes that extend 25 Å out from the contiguous "floor". At the spike tip are two copies of the "immunodominant loop". Previously, the epitopes of seven murine monoclonal antibodies have been identified by cryo-EM analysis of Fab-labeled capsids. All but one are conformational and all but one map around the spike tip. The exception, which is also the tightest-binder, straddles an inter-molecular interface on the floor. Seeking to relate these observations to the immunological response of infected humans, we isolated anti-cAg antibodies from a patient, prepared Fabs, and analyzed their binding to capsids. A priori, one possibility was that many different Fabs would give an undifferentiated continuum of Fab-related density. In fact, the density observed was highly differentiated and could be reproduced by modeling with just five Fabs, three binding to the spike and two to the floor. These results show that epitopes on the floor, far (~30 Å) from the immunodominant loop, are clinically relevant and that murine anti-cAg antibodies afford a good model for the human system., (Published by Elsevier Inc.)

Published

2012

24. Chimeric capsid protein as a nanocarrier for siRNA delivery: stability and cellular uptake of encapsulated siRNA.

Author

Choi KM, Choi SH, Jeon H, Kim IS, and Ahn HJ

Subjects

Amino Acid Sequence, Animals, Capsid Proteins metabolism, Capsid Proteins toxicity, Capsules, Cell Line, Tumor, Cytoplasm metabolism, Drug Carriers chemistry, Drug Carriers metabolism, Drug Carriers toxicity, Gene Silencing, Hepatitis B virus chemistry, Luminescent Proteins genetics, Mice, Models, Molecular, Molecular Sequence Data, Nanostructures toxicity, Protein Conformation, Protein Transport, RNA, Small Interfering blood, RNA, Small Interfering genetics, Recombinant Fusion Proteins metabolism, Recombinant Fusion Proteins toxicity, Red Fluorescent Protein, Capsid Proteins chemistry, Nanostructures chemistry, RNA Stability, RNA, Small Interfering chemistry, RNA, Small Interfering metabolism, Recombinant Fusion Proteins chemistry

Abstract

For the efficient cytoplasmic delivery of siRNA, we designed a chimeric capsid protein composed of a capsid shell, integrin targeting peptide, and p19 RNA binding protein. This recombinant protein assembled into a macromolecular container-like structure with capsid shell and provided a nanocarrier for siRNA delivery. Our capsid nanocarriers had dual affinity both for siRNA within the interior and integin receptors on the exterior, and the capsid shell structure allowed the encapsulated siRNAs to be protected from the external nucleases, leading to the enhanced stability of siRNA in serum conditions. The capsid nanocarriers could complex with siRNA in a size-dependent and sequence-independent manner and showed the pH-dependent complexing/dissocation behaviors with siRNA. Moreover, RGD peptides on the exterior surface of the capsid shell enabled the capsid nanocarriers to deliver siRNA into the cytosol of the target cells. Here, we demonstrated the superior efficiency of our siRNA/capsid nanocarrier complexes in RFP gene silencing, compared to untreated cells. These results provide an alternative approach to enhancing the stability of siRNA as well as to achieving targeted siRNA delivery., (© 2011 American Chemical Society)

Published

2011

25. Interrogating viral capsid assembly with ion mobility-mass spectrometry.

Author

Uetrecht C, Barbu IM, Shoemaker GK, van Duijn E, and Heck AJ

Subjects

Hepatitis B virus chemistry, Hepatitis B virus metabolism, Humans, Models, Molecular, Norovirus chemistry, Norovirus metabolism, Protein Conformation, Capsid chemistry, Capsid metabolism, Capsid Proteins chemistry, Capsid Proteins metabolism, Mass Spectrometry methods, Virus Assembly

Abstract

Most proteins fulfil their function as part of large protein complexes. Surprisingly, little is known about the pathways and regulation of protein assembly. Several viral coat proteins can spontaneously assemble into capsids in vitro with morphologies identical to the native virion and thus resemble ideal model systems for studying protein complex formation. Even for these systems, the mechanism for self-assembly is still poorly understood, although it is generally thought that smaller oligomeric structures form key intermediates. This assembly nucleus and larger viral assembly intermediates are typically low abundant and difficult to monitor. Here, we characterised small oligomers of Hepatitis B virus (HBV) and norovirus under equilibrium conditions using native ion mobility mass spectrometry. This data in conjunction with computational modelling enabled us to elucidate structural features of these oligomers. Instead of more globular shapes, the intermediates exhibit sheet-like structures suggesting that they are assembly competent. We propose pathways for the formation of both capsids.

Published

2011

26. Trapping of hepatitis B virus capsid assembly intermediates by phenylpropenamide assembly accelerators.

Author

Katen SP, Chirapu SR, Finn MG, and Zlotnick A

Subjects

Capsid Proteins ultrastructure, Hepatitis B virus ultrastructure, Kinetics, Microscopy, Electron, Transmission, Molecular Structure, Thermodynamics, Amides chemistry, Capsid Proteins chemistry, Hepatitis B virus chemistry, Hepatitis B virus physiology, Virus Assembly

Abstract

Understanding the biological self-assembly process of virus capsids is key to understanding the viral life cycle, as well as serving as a platform for the design of assembly-based antiviral drugs. Here we identify and characterize the phenylpropenamide family of small molecules, known to have antiviral activity in vivo, as assembly effectors of the hepatitis B virus (HBV) capsid. We have found two representative phenylpropenamides to be assembly accelerators, increasing the rate of assembly with only modest increases in the stability of the HBV capsids; these data provide a physical-chemical basis for their antiviral activity. Unlike previously described HBV assembly effectors, the phenylpropenamides do not misdirect assembly; rather, the accelerated reactions proceed on-path to produce morphologically normal capsids. However, capsid assembly in the presence of phenylpropenamides is characterized by kinetic trapping of assembly intermediates. These traps resolve under conditions close to physiological, but we found that trapped intermediates persist under conditions that favor phenylpropenamide binding and strong core protein-protein interactions. The phenylpropenamides serve as chemical probes of the HBV capsid assembly pathway by trapping on-path assembly intermediates, illustrating the governing influence of reaction kinetics on capsid assembly.

Published

2010

27. Internal core protein cleavage leaves the hepatitis B virus capsid intact and enhances its capacity for surface display of heterologous whole chain proteins.

Author

Walker A, Skamel C, Vorreiter J, and Nassal M

Subjects

Antigens, Surface chemistry, Antigens, Surface genetics, Antigens, Surface immunology, Bacterial Outer Membrane Proteins chemistry, Bacterial Outer Membrane Proteins genetics, Bacterial Outer Membrane Proteins immunology, Bacterial Vaccines chemistry, Bacterial Vaccines genetics, Bacterial Vaccines immunology, Borrelia burgdorferi genetics, Borrelia burgdorferi immunology, Capsid chemistry, Capsid immunology, Capsid ultrastructure, Capsid Proteins chemistry, Capsid Proteins genetics, Capsid Proteins immunology, Endopeptidases biosynthesis, Endopeptidases chemistry, Endopeptidases genetics, Endopeptidases immunology, Epitopes, B-Lymphocyte chemistry, Epitopes, B-Lymphocyte genetics, Epitopes, B-Lymphocyte immunology, Hepatitis B Core Antigens chemistry, Hepatitis B Core Antigens genetics, Hepatitis B Core Antigens immunology, Hepatitis B virus chemistry, Hepatitis B virus genetics, Hepatitis B virus immunology, Lipoproteins chemistry, Lipoproteins genetics, Lipoproteins immunology, Lyme Disease genetics, Lyme Disease immunology, Nanoparticles chemistry, Protein Structure, Secondary genetics, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins immunology, Antigens, Surface biosynthesis, Bacterial Outer Membrane Proteins biosynthesis, Bacterial Vaccines biosynthesis, Capsid metabolism, Capsid Proteins biosynthesis, Epitopes, B-Lymphocyte biosynthesis, Hepatitis B Core Antigens biosynthesis, Hepatitis B virus metabolism, Lipoproteins biosynthesis, Recombinant Proteins biosynthesis

Abstract

Virus capsids find increasing use as nanoparticulate platforms for the surface display of heterologous ligands, including as multivalent vaccine carriers. Presentation on the icosahedral hepatitis B virus capsid (HBcAg) is known to strongly enhance immunogenicity of foreign sequences, most efficiently if they are inserted into the dominant c/e1 B cell epitope, a surface-exposed loop in the center of the constituent core protein primary sequence. Even some complete proteins were successfully inserted but others, e.g. the outer surface protein A (OspA) of the Lyme disease agent Borrelia burgdorferi, impaired formation of capsid-like particles (CLPs). This difference can be rationalized by the requirement for the termini of the insert to fit into the predetermined geometry of the two acceptor sites in the carrier. We reasoned that cleavage of one of the two bonds connecting insert and carrier should relieve these constraints, provided the cleaved protein fragments remain competent to support the particle structure. Indeed, HBcAg CLPs containing a recognition site for tobacco etch virus (TEV) protease in the c/e1 loop remained intact after cleavage, as did CLPs carrying a 65-residue peptide insertion. Most importantly, in situ cleavage of a core-OspA fusion protein by coexpressed TEV protease strongly enhanced CLP formation compared with the uncleaved protein. These data attest to the high structural stability of the HBcAg CLP and they significantly widen its applicability as a carrier for heterologous proteins. This approach should be adaptable to any protein-based particle with surface-exposed yet sequence-internal loops.

Published

2008

28. Stability and shape of hepatitis B virus capsids in vacuo.

Author

Uetrecht C, Versluis C, Watts NR, Wingfield PT, Steven AC, and Heck AJ

Subjects

Capsid ultrastructure, Capsid Proteins ultrastructure, Hepatitis B virus ultrastructure, Protein Conformation, Vacuum, Capsid chemistry, Capsid Proteins chemistry, Hepatitis B virus chemistry, Mass Spectrometry methods

Published

2008

29. Kinetic theory of virus capsid assembly.

Author

van der Schoot P and Zandi R

Subjects

Hepatitis B virus chemistry, Hydrogen-Ion Concentration, Kinetics, Models, Statistical, Models, Theoretical, Thermodynamics, Time Factors, Biophysics methods, Capsid chemistry, Capsid Proteins chemistry, Virus Assembly, Viruses chemistry

Abstract

A phenomenological theory is presented for the kinetics of the in vitro assembly and disassembly of icosahedral virus capsids in solutions of coat proteins. The focus is on conditions where nucleation-type processes can be ignored. We find that the kinetics of assembly is strongly concentration dependent and that the late-stage relaxation time varies as the inverse of the square of the concentration. These findings are corroborated by experimental observations on a number of viruses. Further, our theory shows that hysteresis observed in some experiments could be a direct effect of the kinetics of a high-order mass action law, not necessarily the result of a free energy barrier between assembled and disassembled states.

Published

2007

30. Phosphorylation of hepatitis B virus Cp at Ser87 facilitates core assembly.

Author

Kang HY, Lee S, Park SG, Yu J, Kim Y, and Jung G

Subjects

Amino Acid Sequence, Capsid Proteins chemistry, Capsid Proteins genetics, Capsid Proteins ultrastructure, Cell Line, Tumor, Cyclic AMP-Dependent Protein Kinases metabolism, Hepatitis B virus classification, Hepatitis B virus ultrastructure, Humans, Kinetics, Microscopy, Electron, Transmission, Molecular Sequence Data, Phosphorylation, Protein Binding, Serine genetics, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Surface Plasmon Resonance, Capsid Proteins metabolism, Hepatitis B virus chemistry, Hepatitis B virus metabolism, Serine metabolism, Virus Assembly

Abstract

Protein-protein interactions can be regulated by protein modifications such as phosphorylation. Some of the phosphorylation sites (Ser155, Ser162 and Ser170) of HBV (hepatitis B virus) Cp have been discovered and these sites are implicated in the regulation of viral genome encapsidation, capsid localization and nucleocapsid maturation. In the present report, the dimeric form of HBV Cp was phosphorylated by PKA (protein kinase A), but not by protein kinase C in vitro, and the phosphorylation of dimeric Cp facilitated HBV core assembly. Matrix-assisted laser-desorption ionization-time-of-flight analysis revealed that the HBV Cp was phosphorylated at Ser87 by PKA. This was further confirmed using a mutant HBV Cp with S87G mutation. The S87G mutation inhibited the phosphorylation and, as a result, the in vitro HBV core assembly was not facilitated by PKA. In addition, when either pCMV/FLAG-Core(WT) or pCMV/FLAG-Core(S87G) was transfected into HepG2 cells, few mutant Cps (S87G) assembled into capsids compared with the wild-type (WT) Cps, although the same level of total Cps was expressed in both cases. In conclusion, PKA facilitates HBV core assembly through phosphorylation of the HBV Cp at Ser87.

Published

2006

31. Zinc ions trigger conformational change and oligomerization of hepatitis B virus capsid protein.

Author

Stray SJ, Ceres P, and Zlotnick A

Subjects

Capsid Proteins immunology, Cations, Divalent chemistry, Chlorides chemistry, Enzyme-Linked Immunosorbent Assay, Hepatitis B Core Antigens analysis, Hepatitis B virus immunology, Hepatitis B virus physiology, Kinetics, Light, Peptide Chain Elongation, Translational, Protein Binding, Protein Conformation, Scattering, Radiation, Spectrometry, Fluorescence, Temperature, Zinc metabolism, Zinc Compounds chemistry, Capsid Proteins chemistry, Capsid Proteins metabolism, Hepatitis B virus chemistry, Virus Assembly, Zinc chemistry

Abstract

Assembly of virus particles in infected cells is likely to be a tightly regulated process. Previously, we found that in vitro assembly of hepatitis B virus (HBV) capsid protein is highly dependent on protein and NaCl concentration. Here we show that micromolar concentrations of Zn2+ are sufficient to initiate assembly of capsid protein, whereas other mono- and divalent cations elicited assembly only at millimolar concentrations, similar to those required for NaCl-induced assembly. Altered intrinsic protein fluorescence and highly cooperative binding of at least four Zn2+ ions (KD approximately 7 microM) indicated that binding induced a conformational change in capsid protein. At 37 degrees C, Zn2+ enhanced the initial rate of assembly and produced normal capsids, but it did not alter the extent of assembly at equilibrium. Assembly mediated by high zinc concentrations (> or =300 microM) yielded few capsids but produced a population of oligomers recognized by capsid-specific antibodies, suggesting a kinetically trapped assembly reaction. Comparison of kinetic simulations to in vitro assembly reactions leads us to suggest that kinetic trapping was due to the enhancement of the nucleation rate relative to the elongation rate. Zinc-induced HBV assembly has hallmarks of an allosterically regulated process: ligand binding at one site influences binding at other sites (cooperativity) indicating that binding is associated with conformational change, and binding of ligand alters the biological activity of assembly. We conclude that zinc binding enhances the kinetics of assembly by promoting formation of an intermediate that is readily consumed in the reaction. Free zinc ions may not be the true in vivo activator of assembly, but they provide a model for regulation of assembly.

Published

2004

32. Competing hydrophobic and screened-coulomb interactions in hepatitis B virus capsid assembly.

Author

Kegel WK and Schoot Pv Pv

Subjects

Algorithms, Escherichia coli genetics, Osmolar Concentration, Protein Subunits chemistry, Recombinant Proteins chemistry, Capsid Proteins chemistry, Computer Simulation, Hepatitis B virus chemistry, Hydrophobic and Hydrophilic Interactions, Virus Assembly physiology

Abstract

Recent experiments show that, in the range from approximately 15 to 45 degrees C, an increase in the temperature promotes the spontaneous assembly into capsids of the Escherichia coli-expressed coat proteins of hepatitis B virus. Within that temperature interval, an increase in ionic strength up to five times that of standard physiological conditions also acts to promote capsid assembly. To explain both observations we propose an interaction of mean force between the protein subunits that is the sum of an attractive hydrophobic interaction, driving the self-assembly, and a repulsive electrostatic interaction, opposing the self-assembly. We find that the binding strength of the capsid subunits increases with temperature virtually independently of the ionic strength, and that, at fixed temperature, the binding strength increases with the square root of ionic strength. Both predictions are in quantitative agreement with experiment. We point out the similarities of capsid assembly in general and the micellization of surfactants. Finally we make plausible that electrostatic repulsion between the native core subunits of a large class of virus suppresses the formation in vivo of empty virus capsids, that is, without the presence of the charge-neutralizing nucleic acid.

Published

2004

33. Weak protein-protein interactions are sufficient to drive assembly of hepatitis B virus capsids.

Author

Ceres P and Zlotnick A

Subjects

Dimerization, Kinetics, Protein Conformation, Salts, Sodium Chloride chemistry, Structure-Activity Relationship, Thermodynamics, Capsid Proteins chemistry, Capsid Proteins physiology, Hepatitis B Antigens chemistry, Hepatitis B Antigens physiology, Hepatitis B virus chemistry, Hepatitis B virus physiology, Virus Assembly

Abstract

Hepatitis B virus (HBV) is an enveloped DNA virus with a spherical capsid (or core). The capsid is constructed from 120 copies of the homodimeric capsid protein arranged with T = 4 icosahedral symmetry. We examined in vitro assembly of purified E. coli expressed HBV capsid protein. After equilibration, concentrations of capsid and dimer were evaluated by size exclusion chromatography. The extent of assembly increased as temperature and ionic strength increased. The concentration dependence of capsid assembly conformed to the equilibrium expression: K(capsid) = [capsid]/[dimer](120). Given the known geometry for HBV capsids and dimers, the per capsid assembly energy was partitioned into energy per subunit-subunit contact. We were able to make three major conclusions. (i) Weak interactions (from -2.9 kcal/mol at 21 degrees C in low salt to -4.4 kcal/mol at 37 degrees C in high salt) at each intersubunit contact result in a globally stable capsid; weak intersubunit interactions may be the basis for the phenomenon of capsid breathing. (ii) HBV assembly is characterized by positive enthalpy and entropy. The reaction is entropy-driven, consistent with the largely hydrophobic contacts found in the crystal structure. (iii) Increasing NaCl concentration increases the magnitude of free energy, enthalpy, and entropy, as if ionic strength were increasing the amount of hydrophobic surface buried by assembly. This last point leads us to suggest that salt acts by inducing a conformational change in the dimer from an assembly-inactive form to an assembly-active form. This model of conformational change linked to assembly is consistent with immunological differences between dimer and capsid.

Published

2002