Your search keyword '"Porta, Claudine"' showing total 4 results

1. Structure of Ljungan virus provides insight into genome packaging of this picornavirus

Author

Zhu, Ling, Wang, Xiangxi, Ren, Jingshan, Porta, Claudine, Wenham, Hannah, Ekström, Jens-Ola, Panjwani, Anusha, Knowles, Nick J., Kotecha, Abhay, Siebert, C. Alistair, Lindberg, A. Michael, Fry, Elizabeth E., Rao, Zihe, Tuthill, Tobias J., and Stuart, David I.

Subjects

DNA, Complementary, viruses, Cryoelectron Microscopy, virus diseases, Animals, Nucleic Acid Conformation, Parechovirus, RNA, Viral, Article, Cell Line

Abstract

Picornaviruses are responsible for a range of human and animal diseases, but how their RNA genome is packaged remains poorly understood. A particularly poorly studied group within this family are those that lack the internal coat protein, VP4. Here we report the atomic structure of one such virus, Ljungan virus, the type member of the genus Parechovirus B, which has been linked to diabetes and myocarditis in humans. The 3.78-Å resolution cryo-electron microscopy structure shows remarkable features, including an extended VP1 C terminus, forming a major protuberance on the outer surface of the virus, and a basic motif at the N terminus of VP3, binding to which orders some 12% of the viral genome. This apparently charge-driven RNA attachment suggests that this branch of the picornaviruses uses a different mechanism of genome encapsidation, perhaps explored early in the evolution of picornaviruses., The Ljungan virus is a picornavirus that lacks the internal coat protein VP4, and the packaging of its RNA genome is poorly understood. Here, the authors use cryo-electron microscopy to visualize this virus and suggest that it uses a different mechanism to other viruses for encapsidation of its genome.

Published

2015

2. Structure-based energetics of protein interfaces guides foot-and-mouth disease virus vaccine design.

Author

Kotecha A, Seago J, Scott K, Burman A, Loureiro S, Ren J, Porta C, Ginn HM, Jackson T, Perez-Martin E, Siebert CA, Paul G, Huiskonen JT, Jones IM, Esnouf RM, Fry EE, Maree FF, Charleston B, and Stuart DI

Subjects

Animals, Antibodies, Neutralizing blood, Base Sequence, Capsid Proteins metabolism, Computational Biology methods, Cryoelectron Microscopy, Crystallography, X-Ray, Drug Design, Enzyme-Linked Immunosorbent Assay, Foot-and-Mouth Disease immunology, Foot-and-Mouth Disease Virus immunology, Microscopy, Electron, Molecular Dynamics Simulation, Molecular Sequence Data, Protein Interaction Domains and Motifs, Reverse Transcriptase Polymerase Chain Reaction, Sequence Analysis, DNA, Viral Vaccines immunology, Capsid Proteins chemistry, Foot-and-Mouth Disease prevention & control, Foot-and-Mouth Disease Virus chemistry, Models, Molecular, Viral Vaccines chemistry

Abstract

Virus capsids are primed for disassembly, yet capsid integrity is key to generating a protective immune response. Foot-and-mouth disease virus (FMDV) capsids comprise identical pentameric protein subunits held together by tenuous noncovalent interactions and are often unstable. Chemically inactivated or recombinant empty capsids, which could form the basis of future vaccines, are even less stable than live virus. Here we devised a computational method to assess the relative stability of protein-protein interfaces and used it to design improved candidate vaccines for two poorly stable, but globally important, serotypes of FMDV: O and SAT2. We used a restrained molecular dynamics strategy to rank mutations predicted to strengthen the pentamer interfaces and applied the results to produce stabilized capsids. Structural analyses and stability assays confirmed the predictions, and vaccinated animals generated improved neutralizing-antibody responses to stabilized particles compared to parental viruses and wild-type capsids.

Published

2015

3. Picornavirus uncoating intermediate captured in atomic detail.

Author

Ren J, Wang X, Hu Z, Gao Q, Sun Y, Li X, Porta C, Walter TS, Gilbert RJ, Zhao Y, Axford D, Williams M, McAuley K, Rowlands DJ, Yin W, Wang J, Stuart DI, Rao Z, and Fry EE

Subjects

Animals, Chlorocebus aethiops, Crystallography, X-Ray, Enterovirus, Humans, Models, Molecular, Molecular Conformation, Vero Cells, Viral Structural Proteins chemistry, Virion metabolism, Virus Internalization, Picornaviridae chemistry, Picornaviridae physiology, Virus Uncoating physiology

Abstract

It remains largely mysterious how the genomes of non-enveloped eukaryotic viruses are transferred across a membrane into the host cell. Picornaviruses are simple models for such viruses, and initiate this uncoating process through particle expansion, which reveals channels through which internal capsid proteins and the viral genome presumably exit the particle, although this has not been clearly seen until now. Here we present the atomic structure of an uncoating intermediate for the major human picornavirus pathogen CAV16, which reveals VP1 partly extruded from the capsid, poised to embed in the host membrane. Together with previous low-resolution results, we are able to propose a detailed hypothesis for the ordered egress of the internal proteins, using two distinct sets of channels through the capsid, and suggest a structural link to the condensed RNA within the particle, which may be involved in triggering RNA release.

Published

2013

4. A sensor-adaptor mechanism for enterovirus uncoating from structures of EV71.

Author

Wang X, Peng W, Ren J, Hu Z, Xu J, Lou Z, Li X, Yin W, Shen X, Porta C, Walter TS, Evans G, Axford D, Owen R, Rowlands DJ, Wang J, Stuart DI, Fry EE, and Rao Z

Subjects

Capsid chemistry, Capsid Proteins chemistry, Crystallography, X-Ray, Hand, Foot and Mouth Disease virology, Humans, Models, Molecular, Enterovirus A, Human chemistry, Enterovirus Infections virology, Virion chemistry

Abstract

Enterovirus 71 (EV71) is a major agent of hand, foot and mouth disease in children that can cause severe central nervous system disease and death. No vaccine or antiviral therapy is available. High-resolution structural analysis of the mature virus and natural empty particles shows that the mature virus is structurally similar to other enteroviruses. In contrast, the empty particles are markedly expanded and resemble elusive enterovirus-uncoating intermediates not previously characterized in atomic detail. Hydrophobic pockets in the EV71 capsid are collapsed in this expanded particle, providing a detailed explanation of the mechanism for receptor-binding triggered virus uncoating. These structures provide a model for enterovirus uncoating in which the VP1 GH loop acts as an adaptor-sensor for cellular receptor attachment, converting heterologous inputs to a generic uncoating mechanism, highlighting new opportunities for therapeutic intervention.

Published

2012