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1. Infectious parvovirus B19 circulates in the blood coated with active host protease inhibitors

Author

Hyunwook Lee, Ruben Assaraf, Suriyasri Subramanian, Dan Goetschius, Jan Bieri, Nadia M. DiNunno, Remo Leisi, Carol M. Bator, Susan L. Hafenstein, and Carlos Ros

Subjects
Science
Abstract

Abstract The lack of a permissive cell culture system has limited high-resolution structures of parvovirus B19 (B19V) to virus-like particles (VLPs). In this study, we present the atomic resolution structure (2.2 Å) of authentic B19V purified from a patient blood sample. There are significant differences compared to non-infectious VLPs. Most strikingly, two host protease inhibitors (PIs), inter-alpha-trypsin inhibitor heavy chain 4 (ITIH4) and serpinA3, were identified in complex with the capsids in all patient samples tested. The ITIH4 binds specifically to the icosahedral fivefold axis and serpinA3 occupies the twofold axis. The protein-coated virions remain infectious, and the capsid-associated PIs retain activity; however, upon virion interaction with target cells, the PIs dissociate from the capsid prior to viral entry. Our finding of an infectious virion shielded by bound host serum proteins suggests an evolutionarily favored phenomenon to evade immune surveillance and escape host protease activity.

Published
2024
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2. Intranasal SARS-CoV-2 RBD decorated nanoparticle vaccine enhances viral clearance in the Syrian hamster model

Author

Devanshi R. Patel, Allen M. Minns, Derek G. Sim, Cassandra J. Field, Abigail E. Kerr, Talia A. Heinly, Erin H. Luley, Randall M. Rossi, Carol M. Bator, Ibrahim M. Moustafa, Elizabeth B. Norton, Susan L. Hafenstein, Scott E. Lindner, and Troy C. Sutton

Subjects
vaccines, SARS-CoV-2, hamster, Microbiology, QR1-502
Abstract

ABSTRACTMultiple vaccines have been developed and licensed for severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2). While these vaccines reduce disease severity, they do not prevent infection. To prevent infection and limit transmission, vaccines must be developed that induce immunity in the respiratory tract. Therefore, we performed proof-of-principle studies with an intranasal nanoparticle vaccine against SARS-CoV-2. The vaccine candidate consisted of the self-assembling 60-subunit I3-01 protein scaffold covalently decorated with the SARS-CoV-2 receptor-binding domain (RBD) using the SpyCatcher-SpyTag system. We verified the intended antigen display features by reconstructing the I3-01 scaffold to 3.4 A using cryogenicelectron microscopy. Using this RBD-grafted SpyCage scaffold (RBD + SpyCage), we performed two intranasal vaccination studies in the “gold-standard” pre-clinical Syrian hamster model. The initial study focused on assessing the immunogenicity of RBD + SpyCage combined with the LTA1 intranasal adjuvant. These studies showed RBD + SpyCage vaccination induced an antibody response that promoted viral clearance but did not prevent infection. Inclusion of the LTA1 adjuvant enhanced the magnitude of the antibody response but did not enhance protection. Thus, in an expanded study, in the absence of an intranasal adjuvant, we evaluated if covalent bonding of RBD to the scaffold was required to induce an antibody response. Covalent grafting of RBD was required for the vaccine to be immunogenic, and animals vaccinated with RBD + SpyCage more rapidly cleared SARS-CoV-2 from both the upper and lower respiratory tract. These findings demonstrate the intranasal SpyCage vaccine platform can induce protection against SARS-CoV-2 and, with additional modifications to improve immunogenicity, is a versatile platform for the development of intranasal vaccines targeting respiratory pathogens.IMPORTANCEDespite the availability of efficacious COVID vaccines that reduce disease severity, SARS-CoV-2 continues to spread. To limit SARS-CoV-2 transmission, the next generation of vaccines must induce immunity in the mucosa of the upper respiratory tract. Therefore, we performed proof-of-principle, intranasal vaccination studies with a recombinant protein nanoparticle scaffold, SpyCage, decorated with the RBD of the S protein (SpyCage + RBD). We show that SpyCage + RBD was immunogenic and enhanced SARS-CoV-2 clearance from the nose and lungs of Syrian hamsters. Moreover, covalent grafting of the RBD to the scaffold was required to induce an immune response when given via the intranasal route. These proof-of-concept findings indicate that with further enhancements to immunogenicity (e.g., adjuvant incorporation and antigen optimization), the SpyCage scaffold has potential as a versatile, intranasal vaccine platform for respiratory pathogens.

Published
2024
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3. A human monoclonal antibody binds within the poliovirus receptor-binding site to neutralize all three serotypes

Author

Andrew J. Charnesky, Julia E. Faust, Hyunwook Lee, Rama Devudu Puligedda, Daniel J. Goetschius, Nadia M. DiNunno, Vaskar Thapa, Carol M. Bator, Sung Hyun (Joseph) Cho, Rahnuma Wahid, Kutub Mahmood, Scott Dessain, Konstantin M. Chumakov, Amy Rosenfeld, and Susan L. Hafenstein

Subjects
Science
Abstract

Abstract Global eradication of poliovirus remains elusive, and it is critical to develop next generation vaccines and antivirals. In support of this goal, we map the epitope of human monoclonal antibody 9H2 which is able to neutralize the three serotypes of poliovirus. Using cryo-EM we solve the near-atomic structures of 9H2 fragments (Fab) bound to capsids of poliovirus serotypes 1, 2, and 3. The Fab-virus complexes show that Fab interacts with the same binding mode for each serotype and at the same angle of interaction relative to the capsid surface. For each of the Fab-virus complexes, we find that the binding site overlaps with the poliovirus receptor (PVR) binding site and maps across and into a depression in the capsid called the canyon. No conformational changes to the capsid are induced by Fab binding for any complex. Competition binding experiments between 9H2 and PVR reveal that 9H2 impedes receptor binding. Thus, 9H2 outcompetes the receptor to neutralize poliovirus. The ability to neutralize all three serotypes, coupled with the critical importance of the conserved receptor binding site make 9H2 an attractive antiviral candidate for future development.

Published
2023
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4. Cryo EM structures map a post vaccination polyclonal antibody response to canine parvovirus

Author

Samantha R. Hartmann, Andrew J. Charnesky, Simon P. Früh, Robert A. López-Astacio, Wendy S. Weichert, Nadia DiNunno, Sung Hung Cho, Carol M. Bator, Colin R. Parrish, and Susan L. Hafenstein

Subjects
Biology (General), QH301-705.5
Abstract

Abstract Canine parvovirus (CPV) is an important pathogen that emerged by cross-species transmission to cause severe disease in dogs. To understand the host immune response to vaccination, sera from dogs immunized with parvovirus are obtained, the polyclonal antibodies are purified and used to solve the high resolution cryo EM structures of the polyclonal Fab-virus complexes. We use a custom software, Icosahedral Subparticle Extraction and Correlated Classification (ISECC) to perform subparticle analysis and reconstruct polyclonal Fab-virus complexes from two different dogs eight and twelve weeks post vaccination. In the resulting polyclonal Fab-virus complexes there are a total of five distinct Fabs identified. In both cases, any of the five antibodies identified would interfere with receptor binding. This polyclonal mapping approach identifies a specific, limited immune response to the live vaccine virus and allows us to investigate the binding of multiple different antibodies or ligands to virus capsids.

Published
2023
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5. High resolution cryo EM analysis of HPV16 identifies minor structural protein L2 and describes capsid flexibility

Author

Daniel J. Goetschius, Samantha R. Hartmann, Suriyasri Subramanian, Carol M. Bator, Neil D. Christensen, and Susan L. Hafenstein

Subjects
Medicine, Science
Abstract

Abstract Human papillomavirus (HPV) is a significant health burden and leading cause of virus-induced cancers. HPV is epitheliotropic and its replication is tightly associated with terminal keratinocyte differentiation making production and purification of high titer virus preparations for research problematic, therefore alternative HPV production methods have been developed for virological and structural studies. In this study we use HPV16 quasivirus, composed of HPV16 L1/L2 capsid proteins with a packaged cottontail rabbit papillomavirus genome. We have achieved the first high resolution, 3.1 Å, structure of HPV16 by using a local subvolume refinement approach. The high resolution enabled us to build L1 unambiguously and identify L2 protein strands. The L2 density is incorporated adjacent to conserved L1 residues on the interior of the capsid. Further interpretation with our own software for Icosahedral Subvolume Extraction and Correlated Classification revealed flexibility, on the whole-particle level through diameter analysis and local movement with inter-capsomer analysis. Inter-capsomer expansion or contraction, governed by the connecting arms, showed no bias in the magnitude or direction of capsomer movement. We propose that papillomavirus capsids are dynamic and capsomers move as rigid bodies connected by flexible linkers. The resulting virus structure will provide a framework for continuing biochemical, genetic and biophysical research for papillomaviruses. Furthermore, our approach has allowed insight into the resolution barrier that has previously been a limitation in papillomavirus structural studies.

Published
2021
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6. Identification of a pocket factor that is critical to Zika virus assembly

Author

Nadia M. DiNunno, Daniel J. Goetschius, Anoop Narayanan, Sydney A. Majowicz, Ibrahim Moustafa, Carol M. Bator, Susan L. Hafenstein, and Joyce Jose

Subjects
Science
Abstract

Here, the authors provide a 3.4 Å resolution structure of mature Zika virus (ZIKV) and identify two lipid moieties, coordinated by hydrophobic residues of the M and E transmembrane helices and between two helices of E protein, that play an essential role in the ZIKV assembly pathway.

Published
2020
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7. Cryo EM Analysis Reveals Inherent Flexibility of Authentic Murine Papillomavirus Capsids

Author

Samantha R. Hartmann, Daniel J. Goetschius, Jiafen Hu, Joshua J. Graff, Carol M. Bator, Neil D. Christensen, and Susan L. Hafenstein

Subjects
mouse papillomavirus, cryo EM, HPV16, Microbiology, QR1-502
Abstract

Human papillomavirus (HPV) is a significant health burden and leading cause of virus-induced cancers. However, studies have been hampered due to restricted tropism that makes production and purification of high titer virus problematic. This issue has been overcome by developing alternative HPV production methods such as virus-like particles (VLPs), which are devoid of a native viral genome. Structural studies have been limited in resolution due to the heterogeneity, fragility, and stability of the VLP capsids. The mouse papillomavirus (MmuPV1) presented here has provided the opportunity to study a native papillomavirus in the context of a common laboratory animal. Using cryo EM to solve the structure of MmuPV1, we achieved 3.3 Å resolution with a local symmetry refinement method that defined smaller, symmetry related subparticles. The resulting high-resolution structure allowed us to build the MmuPV1 asymmetric unit for the first time and identify putative L2 density. We also used our program ISECC to quantify capsid flexibility, which revealed that capsomers move as rigid bodies connected by flexible linkers. The MmuPV1 flexibility was comparable to that of a HPV VLP previously characterized. The resulting MmuPV1 structure is a promising step forward in the study of papillomavirus and will provide a framework for continuing biochemical, genetic, and biophysical research for papillomaviruses.

Published
2021
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8. Antibody escape by polyomavirus capsid mutation facilitates neurovirulence

Author

Matthew D Lauver, Daniel J Goetschius, Colleen S Netherby-Winslow, Katelyn N Ayers, Ge Jin, Daniel G Haas, Elizabeth L Frost, Sung Hyun Cho, Carol M Bator, Stephanie M Bywaters, Neil D Christensen, Susan L Hafenstein, and Aron E Lukacher

Subjects
polyomavirus, neutralizing antibody, progressive multifocal leukoencephalopathy, Cryo EM, subvolume refinement, fab:capsid complex, Medicine, Science, Biology (General), QH301-705.5
Abstract

JCPyV polyomavirus, a member of the human virome, causes progressive multifocal leukoencephalopathy (PML), an oft-fatal demyelinating brain disease in individuals receiving immunomodulatory therapies. Mutations in the major viral capsid protein, VP1, are common in JCPyV from PML patients (JCPyV-PML) but whether they confer neurovirulence or escape from virus-neutralizing antibody (nAb) in vivo is unknown. A mouse polyomavirus (MuPyV) with a sequence-equivalent JCPyV-PML VP1 mutation replicated poorly in the kidney, a major reservoir for JCPyV persistence, but retained the CNS infectivity, cell tropism, and neuropathology of the parental virus. This mutation rendered MuPyV resistant to a monoclonal Ab (mAb), whose specificity overlapped the endogenous anti-VP1 response. Using cryo-EM and a custom sub-particle refinement approach, we resolved an MuPyV:Fab complex map to 3.2 Å resolution. The structure revealed the mechanism of mAb evasion. Our findings demonstrate convergence between nAb evasion and CNS neurovirulence in vivo by a frequent JCPyV-PML VP1 mutation.

Published
2020
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9. Cryo-EM Structure of Gokushovirus ΦEC6098 Reveals a Novel Capsid Architecture for a Single-Scaffolding Protein, Microvirus Assembly System

Author

Hyunwook Lee, Alexis J. Baxter, Carol M. Bator, Bentley A. Fane, and Susan L. Hafenstein

Subjects
Capsid, Virus Assembly, Structure and Assembly, Virology, Insect Science, Cryoelectron Microscopy, Microviridae, Immunology, Capsid Proteins, Microvirus, Microbiology, Ecosystem, Bacteriophage phi X 174
Abstract

Ubiquitous and abundant in ecosystems and microbiomes, gokushoviruses constitute a Microviridae subfamily, distantly related to bacteriophages ΦX174, α3, and G4. A high-resolution cryo-EM structure of gokushovirus ΦEC6098 was determined, and the atomic model was built de novo. Although gokushoviruses lack external scaffolding and spike proteins, which extensively interact with the ΦX174 capsid protein, the core of the ΦEC6098 coat protein (VP1) displayed a similar structure. There are, however, key differences. At each ΦEC6098 icosahedral 3-fold axis, a long insertion loop formed mushroom-like protrusions, which have been noted in lower-resolution gokushovirus structures. Hydrophobic interfaces at the bottom of these protrusions may confer stability to the capsid shell. In ΦX174, the N-terminus of the capsid protein resides directly atop the 3-fold axes of symmetry; however, the ΦEC6098 N-terminus stretched across the inner surface of the capsid shell, reaching nearly to the 5-fold axis of the neighboring pentamer. Thus, this extended N-terminus interconnected pentamers on the inside of the capsid shell, presumably promoting capsid assembly, a function performed by the ΦX174 external scaffolding protein. There were also key differences between the ΦX174-like DNA-binding J proteins and its ΦEC6098 homologue VP8. As seen with the J proteins, C-terminal VP8 residues were bound into a pocket within the major capsid protein; however, its N-terminal residues were disordered, likely due to flexibility. We show that the combined location and interaction of VP8’s C-terminus and a portion of VP1’s N-terminus are reminiscent of those seen with the ΦX174 and α3 J proteins. IMPORTANCE There is a dramatic structural and morphogenetic divide within the Microviridae. The well-studied ΦX174-like viruses have prominent spikes at their icosahedral vertices, which are absent in gokushoviruses. Instead, gokushovirus major coat proteins form extensive mushroom-like protrusions at the 3-fold axes of symmetry. In addition, gokushoviruses lack an external scaffolding protein, the more critical of the two ΦX174 assembly proteins, but retain an internal scaffolding protein. The ΦEC6098 virion suggests that key external scaffolding functions are likely performed by coat protein domains unique to gokushoviruses. Thus, within one family, different assembly paths have been taken, demonstrating how a two-scaffolding protein system can evolve into a one-scaffolding protein system, or vice versa.

Published
2022

10. Imaging 0.36 nm Lattice Planes in Conjugated Polymers by Minimizing Beam Damage

Author

Carol M. Bator, Enrique D. Gomez, and Brooke Kuei

Subjects
chemistry.chemical_classification, Materials science, Polymers and Plastics, business.industry, Organic Chemistry, food and beverages, 02 engineering and technology, Polymer, Conjugated system, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, Soft materials, 0104 chemical sciences, Inorganic Chemistry, chemistry, Transmission electron microscopy, Lattice (order), Materials Chemistry, Optoelectronics, 0210 nano-technology, High-resolution transmission electron microscopy, business
Abstract

Transmission electron microscopy can resolve the atomic structure of materials with 0.5 A resolution. High-resolution transmission electron microscopy (HRTEM) of soft materials, however, is limited...

Published
2020

11. Thioether-Based Polymeric Micelles with Fine-Tuned Oxidation Sensitivities for Chemotherapeutic Drug Delivery

Author

Masoud Ghasemi, Bin Liu, Enrique D. Gomez, Urara Hasegawa, André J. van der Vlies, Jiayi Xu, Amanda Bell, Brett Rosoff-Verbit, and Carol M. Bator

Subjects
Polymers and Plastics, Cell Survival, Substituent, Bioengineering, Sulfides, Micelle, Redox, Article, Biomaterials, chemistry.chemical_compound, Drug Delivery Systems, Thioether, Materials Chemistry, Humans, Reactivity (chemistry), Hydrogen peroxide, Micelles, Drug Carriers, Endothelial Cells, Hydrogen Peroxide, Hydrogen-Ion Concentration, Combinatorial chemistry, Drug Liberation, Thiomorpholine, chemistry, Doxorubicin, Drug delivery
Abstract

Oxidation-sensitive drug delivery systems (DDS) have attracted attention due to the potential to improve efficacy and safety of chemotherapeutics. These systems are designed to release the payload in response to oxidative stress conditions, which are associated with many types of cancer. Despite extensive research on the development of oxidation-sensitive DDS, the lack of selectivity towards cancer cells over healthy cells remains a challenge. Here, we report the design and characterization of polymeric micelles containing thioether groups with varying oxidation sensitivities within the micellar core, which become hydrophilic upon thioether oxidation leading to destabilization of the micellar structure. We first used the thioether model compounds, 3-methylthiopropylamide (TPAM), thiomorpholine amide (TMAM), and 4-(methylthio)benzylamide (TPhAM), to investigate the effect of the chemical structures of the thioethers on the oxidation by hydrogen peroxide [Formula: see text]. TPAM shows the fastest oxidation followed by TMAM and TPhAM, showing that the oxidation reaction of thioethers can be modulated by changing the substituent groups bound to the sulfur atom. We next prepared micelles containing these different thioether groups within the core (TP, TM and TPh micelles). The micelles containing the thioether groups with a higher oxidation sensitivity were destabilized by [Formula: see text] at lower concentration. Micelle destabilization was also tested in human liver cancer (HepG2) cells and human umbilical vein endothelial cells (HUVECs). The TP micelles having the highest oxidation sensitivity were destabilized in both HepG2 cells and HUVECs while the TPh micelles, which showed the lowest reactivity towards [Formula: see text] , were stable in those cell lines. The TM micelles possessing a moderate oxidation sensitivity were destabilized in HepG2 cells but were stable in HUVECs. Furthermore, the micelles were loaded with doxorubicin (Dox) to evaluate their potential in drug delivery applications. Among the micelles, the TM micelles loaded with Dox showed the enhanced relative toxicity in HepG2 cells over HUVECs. Therefore, our approach to fine-tune the oxidation sensitivity of the micelles has potential for improving therapeutic efficacy and safety of drugs in cancer treatment.

Published
2021

12. Cryo EM Analysis Reveals Inherent Flexibility of Authentic Murine Papillomavirus Capsids

Author

Carol M. Bator, Neil D. Christensen, Samantha R. Hartmann, Joshua J. Graff, Susan Hafenstein, Jiafen Hu, and Daniel J. Goetschius

Subjects
Models, Molecular, HPV16, Cryo-electron microscopy, viruses, cryo EM, Context (language use), Computational biology, Genome, Viral, Biology, Genome, Microbiology, Article, Mice, Capsid, Virology, Animals, High titer, Papillomaviridae, Tropism, Flexibility (engineering), Capsomere, Cryoelectron Microscopy, Papillomavirus Infections, virus diseases, Oncogene Proteins, Viral, QR1-502, mouse papillomavirus, Infectious Diseases, Viruses, Unclassified, Capsid Proteins
Abstract

Human papillomavirus (HPV) is a significant health burden and leading cause of virus-induced cancers. However, studies have been hampered due to restricted tropism that makes production and purification of high titer virus problematic. This issue has been overcome by developing alternative HPV production methods such as virus-like particles (VLPs), which are devoid of a native viral genome. Structural studies have been limited in resolution due to the heterogeneity, fragility, and stability of the VLP capsids. The mouse papillomavirus (MmuPV1) presented here has provided the opportunity to study a native papillomavirus in the context of a common laboratory animal. Using cryo EM to solve the structure of MmuPV1, we achieved 3.3 Å resolution with a local symmetry refinement method that defined smaller, symmetry related subparticles. The resulting high-resolution structure allowed us to build the MmuPV1 asymmetric unit for the first time and identify putative L2 density. We also used our program ISECC to quantify capsid flexibility, which revealed that capsomers move as rigid bodies connected by flexible linkers. The MmuPV1 flexibility was comparable to that of a HPV VLP previously characterized. The resulting MmuPV1 structure is a promising step forward in the study of papillomavirus and will provide a framework for continuing biochemical, genetic, and biophysical research for papillomaviruses.

Published
2021
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13. Rapid preparation of nanodiscs for biophysical studies

Author

Esther W. Gomez, Kerney Jebrell Glover, Enrique D. Gomez, Katrina M. Brandmier, Joshua T. Del Mundo, Jeffrey A. Julien, Martin G. Fernandez, Carol M. Bator, and Lucie A. Loftus

Subjects
Protein Conformation, alpha-Helical, Circular dichroism, Chemistry, Lipid Bilayers, Size-exclusion chromatography, Biophysics, Membrane Proteins, Biochemistry, Article, Nanostructures, Molecular Weight, Analytical Ultracentrifugation, Membrane, Dynamic light scattering, Amphiphile, Particle Size, Dimyristoylphosphatidylcholine, Dialysis (biochemistry), Lipid bilayer, Molecular Biology
Abstract

Nanodiscs, which are disc-shaped entities that contain a central lipid bilayer encased by an annulus of amphipathic helices, have emerged as a leading native-like membrane mimic. The current approach for the formation of nanodiscs involves the creation of a mixed-micellar solution containing membrane scaffold protein, lipid, and detergent followed by a time consuming process (3-12 h) of dialysis and/or incubation with sorptive beads to remove the detergent molecules from the sample. In contrast, the methodology described herein provides a facile and rapid procedure for the preparation of nanodiscs in a matter of minutes (

Published
2021

14. Transferrin receptor binds virus capsid with dynamic motion

Author

Colin R. Parrish, Susan Hafenstein, Carol M. Bator, Hyunwook Lee, Javier O. Cifuente, and Heather M. Callaway

Subjects
Parvovirus, Canine, Protein Conformation, animal diseases, viruses, Transferrin receptor, Virus, 03 medical and health sciences, Capsid, Dogs, Species Specificity, Receptors, Transferrin, Animals, Binding site, Receptor, Pathogen, 030304 developmental biology, Dynamic motion, 0303 health sciences, Multidisciplinary, biology, 030306 microbiology, Chemistry, Cryoelectron Microscopy, Virion, Canine parvovirus, biology.organism_classification, Cell biology, PNAS Plus, Cats, Receptors, Virus
Abstract

Canine parvovirus (CPV) is an important pathogen causing severe diseases in dogs, including acute hemorrhagic enteritis, myocarditis, and cerebellar disease. Cross-species transmission of CPV occurs as a result of mutations on the viral capsid surface that alter the species-specific binding to the host receptor, transferrin receptor type-1 (TfR). The interaction between CPV and TfR has been extensively studied, and previous analyses have suggested that the CPV–TfR complex is asymmetric. To enhance the understanding of the underlying molecular mechanisms, we determined the CPV–TfR interaction using cryo-electron microscopy to solve the icosahedral (3.0-Å resolution) and asymmetric (5.0-Å resolution) complex structures. Structural analyses revealed conformational variations of the TfR molecules relative to the binding site, which translated into dynamic molecular interactions between CPV and TfR. The precise footprint of the receptor on the virus capsid was identified, along with the identity of the amino acid residues in the virus–receptor interface. Our “rock-and-roll” model provides an explanation for previous findings and gives insights into species jumping and the variation in host ranges associated with new pandemics in dogs.

Published
2019

15. High-resolution asymmetric structure of a Fab–virus complex reveals overlap with the receptor binding site

Author

James F. Conway, Carol M. Bator, Daniel J. Goetschius, Susan Hafenstein, Robert E. Ashley, Alexander M. Makhov, Kai Huang, Lindsey J. Organtini, Samantha R. Hartmann, Colin R. Parrish, and Heather M. Callaway

Subjects
Parvovirus, Canine, Cryo-electron microscopy, medicine.drug_class, viruses, ISECC, Antibodies, Viral, Monoclonal antibody, Microbiology, Virus, Epitope, Epitopes, Immunoglobulin Fab Fragments, 03 medical and health sciences, Capsid, Dogs, Protein Domains, medicine, Animals, Antigens, 030304 developmental biology, epitope, 0303 health sciences, Binding Sites, Multidisciplinary, biology, 030306 microbiology, Parvovirus, Chemistry, parvovirus, Cryoelectron Microscopy, Canine parvovirus, Biological Sciences, biology.organism_classification, virus–fab complex, Mutation, Biophysics, cryo-EM, Protein Binding, Conformational epitope
Abstract

Significance Our study makes significant progress understanding asymmetry in icosahedral viruses that would be otherwise masked by forcing homogeneity through icosahedral averaging. Using an asymmetric approach revealed the atomic-resolution structure of a complex between canine parvovirus and a strain-specific neutralizing antibody. Since species jumping is a rare event in DNA viruses, the emergence of an antibody that binds more avidly to the canine-adapted virus (and not ancestral feline equivalent) is of special interest. The Fab-bound and -unbound epitopes were solved on the same virus capsid with an atomic-resolution asymmetric map. Fab 14 stabilizes a capsid loop within the same binding site used by the receptor, suggesting capsid conformational change or steric competition with the receptor contributes to the mechanism of antibody neutralization., Canine parvovirus is an important pathogen causing severe diseases in dogs, including acute hemorrhagic enteritis, myocarditis, and cerebellar disease. Overlap on the surface of parvovirus capsids between the antigenic epitope and the receptor binding site has contributed to cross-species transmission, giving rise to closely related variants. It has been shown that Mab 14 strongly binds and neutralizes canine but not feline parvovirus, suggesting this antigenic site also controls species-specific receptor binding. To visualize the conformational epitope at high resolution, we solved the cryogenic electron microscopy (cryo-EM) structure of the Fab–virus complex. We also created custom software, Icosahedral Subparticle Extraction and Correlated Classification, to solve a Fab–virus complex with only a few Fab bound per capsid and visualize local structures of the Fab-bound and -unbound antigenic sites extracted from the same complex map. Our results identified the antigenic epitope that had significant overlap with the receptor binding site, and the structures revealed that binding of Fab induced conformational changes to the virus. We were also able to assign the order and position of attached Fabs to allow assessment of complementarity between the Fabs bound to different positions. This approach therefore provides a method for using cryo-EM to investigate complementarity of antibody binding.

Published
2021

16. High resolution cryo EM analysis of HPV16 identifies minor structural protein L2 and describes capsid flexibility

Author

Susan Hafenstein, Carol M. Bator, Suriyasri Subramanian, Neil D. Christensen, Samantha R. Hartmann, and Daniel J. Goetschius

Subjects
0301 basic medicine, Models, Molecular, Flexibility (anatomy), Cryo-electron microscopy, Science, viruses, Computational biology, Human papilloma virus, Biology, Genome, Virus, Article, 03 medical and health sciences, Epitopes, 0302 clinical medicine, Capsid, Cryoelectron microscopy, medicine, Humans, Papillomaviridae, Human papillomavirus 16, Multidisciplinary, Capsomere, Resolution (electron density), Cottontail rabbit papillomavirus, Virion, virus diseases, Oncogene Proteins, Viral, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Medicine, Capsid Proteins, Protein Binding
Abstract

Human papillomavirus (HPV) is a significant health burden and leading cause of virus-induced cancers. HPV is epitheliotropic and its replication is tightly associated with terminal keratinocyte differentiation making production and purification of high titer virus preparations for research problematic, therefore alternative HPV production methods have been developed for virological and structural studies. In this study we use HPV16 quasivirus, composed of HPV16 L1/L2 capsid proteins with a packaged cottontail rabbit papillomavirus genome. We have achieved the first high resolution, 3.1Å, structure of HPV16 by using a local subvolume refinement approach. The high resolution enabled us to build L1 unambiguously and identify L2 protein strands. The L2 density is incorporated adjacent to conserved L1 residues on the interior of the capsid. Further interpretation with our own software for Icosahedral Subvolume Extraction and Correlated Classification (ISECC) revealed flexibility, on the whole-particle level through diameter analysis and local movement with inter-capsomer analysis. Inter-capsomer expansion or contraction, governed by the connecting arms, showed no bias in the magnitude or direction of capsomer movement. We propose that papillomavirus capsids are dynamic and capsomers move as rigid bodies connected by flexible linkers. The resulting virus structure will provide a framework for continuing biochemical, genetic and biophysical research for papillomaviruses. Furthermore, our approach has allowed insight into the resolution barrier that has previously been a limitation in papillomavirus structural studies.

Published
2020

17. Identification of a pocket factor that is critical to Zika virus assembly

Author

Daniel J. Goetschius, Joyce Jose, Nadia M. DiNunno, Carol M. Bator, Anoop Narayanan, Ibrahim M. Moustafa, Susan Hafenstein, and Sydney A. Majowicz

Subjects
0301 basic medicine, Science, General Physics and Astronomy, Mutagenesis (molecular biology technique), General Biochemistry, Genetics and Molecular Biology, Virus, Article, Zika virus, Hydrophobic effect, 03 medical and health sciences, 0302 clinical medicine, Viral life cycle, Cryoelectron microscopy, Chlorocebus aethiops, Animals, Humans, Lipid bilayer, lcsh:Science, Vero Cells, Multidisciplinary, biology, Chemistry, Virus Assembly, Virion, General Chemistry, Zika Virus, Virus structures, biology.organism_classification, Cell biology, Transmembrane domain, Flavivirus, 030104 developmental biology, HEK293 Cells, lcsh:Q, 030217 neurology & neurosurgery
Abstract

Zika virus (ZIKV) is an emerging mosquito borne flavivirus and a major public health concern causing severe disease. Due to the presence of a lipid membrane and structural heterogeneity, attaining an atomic resolution structure is challenging, but important to understand virus assembly and life cycle mechanisms that offer distinct targets for therapeutic intervention. We here use subvolume refinement to achieve a 3.4 Å resolution structure and identify two distinct lipid moieties. The first arises from the inner leaflet and is coordinated by hydrophobic residues of the M and E transmembrane helices that form a binding pocket not previously characterized. The second lipid arises from the outer leaflet coordinate between two E protein helices. Structure-based mutagenesis identifies critical hydrophobic interactions and their effect on the virus life cycle. Results show that lipids play an essential role in the ZIKV assembly pathway revealing a potential target of lipid based antiviral drug development., Here, the authors provide a 3.4 Å resolution structure of mature Zika virus (ZIKV) and identify two lipid moieties, coordinated by hydrophobic residues of the M and E transmembrane helices and between two helices of E protein, that play an essential role in the ZIKV assembly pathway.

Published
2020

18. Author response: Antibody escape by polyomavirus capsid mutation facilitates neurovirulence

Author

Stephanie M. Bywaters, Colleen S. Netherby-Winslow, Daniel G Haas, Daniel J. Goetschius, Ge Jin, Elizabeth L. Frost, Sung Hyun Cho, Susan Hafenstein, Carol M. Bator, Aron E. Lukacher, Neil D. Christensen, Katelyn N. Ayers, and Matthew D. Lauver

Subjects
biology, Capsid, Mutation (genetic algorithm), biology.protein, Antibody, Virology
Published
2020

19. Enhanced Surface Activity of MWW Zeolite Nanosheets Prepared via a One-Step Synthesis

Author

Bernd Kabius, Yunwen Zhou, Carlos Pacheco, Jeffrey D. Rimer, Carol M. Bator, Ming-Feng Hsieh, Yanyu Mu, and Robert M. Rioux

Subjects
Chemistry, One-Step, General Chemistry, 010402 general chemistry, 01 natural sciences, Biochemistry, Exfoliation joint, Catalysis, 0104 chemical sciences, Colloid and Surface Chemistry, Template, Chemical engineering, Molecule, Selectivity, Brønsted–Lowry acid–base theory, Zeolite
Abstract

The synthesis of two-dimensional (2D) zeolites has garnered attention due to their superior properties for applications that span catalysis to selective separations. Prior studies of 2D zeolite catalysts demonstrated enhanced mass transport for improved catalyst lifetime and selectivity. Moreover, the significantly higher external surface area of 2D materials allows for reactions of bulky molecules too large to access interior pores. There are relatively few protocols for preparing 2D materials, owing to the difficultly of capping growth in one direction to only a few unit cells. To accomplish this, it is often necessary to employ complex, commercially unavailable organic structure-directing agents (OSDAs) prepared via multistep synthesis. However, a small subset of zeolite structures exist as naturally layered materials where postsynthesis steps can be used to exfoliate samples and produce ultrathin 2D nanosheets. In this study, we selected a common layered zeolite, the MWW framework, to explore methods of preparing 2D nanosheets via one-pot synthesis in the absence of complex organic templates. Using a combination of high-resolution microscopy and spectroscopy, we show that 2D MMW-type layers with an average thickness of 3.5 nm (ca. 1.5 unit cells) can be generated using the surfactant cetyltrimethylammonium (CTA), which operates as a dual OSDA and exfoliating agent to affect Al siting and to eliminate the need for postsynthesis exfoliation, respectively. We tested these 2D catalysts using a model reaction that assesses external (surface) Bronsted acid sites and observed a marked increase in the conversion relative to three-dimensional MWW (MCM-22) and 2D layers prepared from postsynthesis exfoliation (ITQ-2). Collectively, our findings identify a facile and effective route to directly synthesize 2D MWW-type materials, which may prove to be more broadly applicable to other layered zeolites.

Published
2020

20. Cryo-EM structure of catalytic ribonucleoprotein complex RNase MRP

Author

Di Li, Susan Hafenstein, Anna Perederina, Igor Berezin, Hyunwook Lee, Andrey S. Krasilnikov, and Carol M. Bator

Subjects
Models, Molecular, 0301 basic medicine, Protein Conformation, Cryo-electron microscopy, RNase P, Science, General Physics and Astronomy, Saccharomyces cerevisiae, Catalysis, Ribonuclease P, General Biochemistry, Genetics and Molecular Biology, Ribonucleoprotein complex, 03 medical and health sciences, 0302 clinical medicine, stomatognathic system, Catalytic Domain, Endoribonucleases, Humans, RNA, Catalytic, lcsh:Science, chemistry.chemical_classification, Multidisciplinary, biology, Chemistry, Cryoelectron Microscopy, Ribozyme, RNA, RNA, Fungal, General Chemistry, Ribosomal RNA, Cell cycle, Carbon, Cell biology, RNase MRP, 030104 developmental biology, Enzyme, Ribonucleoproteins, biology.protein, Nucleic Acid Conformation, lcsh:Q, 030217 neurology & neurosurgery
Abstract

RNase MRP is an essential eukaryotic ribonucleoprotein complex involved in the maturation of rRNA and the regulation of the cell cycle. RNase MRP is related to the ribozyme-based RNase P, but it has evolved to have distinct cellular roles. We report a cryo-EM structure of the S. cerevisiae RNase MRP holoenzyme solved to 3.0 A. We describe the structure of this 450 kDa complex, interactions between its components, and the organization of its catalytic RNA. We show that some of the RNase MRP proteins shared with RNase P undergo an unexpected RNA-driven remodeling that allows them to bind to divergent RNAs. Further, we reveal how this RNA-driven protein remodeling, acting together with the introduction of new auxiliary elements, results in the functional diversification of RNase MRP and its progenitor, RNase P, and demonstrate structural underpinnings of the acquisition of new functions by catalytic RNPs. Ribozyme-based RNase MRP is an essential eukaryotic enzyme involved in the maturation of rRNA and is evolutionarily related to RNase P. Here, the authors present the 3.0 A cryo-EM structure of the S. cerevisiae RNase MRP holoenzyme, a 450 kDa ribonucleoprotein complex and compare it with RNase P.

Published
2020
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21. Scaffold Simplification Strategy Leads to a Novel Generation of Dual Human Immunodeficiency Virus and Enterovirus-A71 Entry Inhibitors

Author

María-José Camarasa, Dominique Schols, Hyunwook Lee, Ernesto Quesada, Olaia Martí-Marí, Belén Martínez-Gualda, Johan Neyts, Carol M. Bator, Rana Abdelnabi, Liang Sun, Federico Gago, Sam Noppen, Carmen Mirabelli, Leen Delang, Susan Hafenstein, Ana San-Félix, Ministerio de Economía y Competitividad (España), Agencia Estatal de Investigación (España), European Commission, Consejo Superior de Investigaciones Científicas (España), University of Leuven, and China Scholarship Council

Subjects
Drug, CD4-Positive T-Lymphocytes, Models, Molecular, Scaffold, viruses, media_common.quotation_subject, Human immunodeficiency virus (HIV), Disease, Microbial Sensitivity Tests, medicine.disease_cause, Virus Replication, 01 natural sciences, Antiviral Agents, Virus, 03 medical and health sciences, Structure-Activity Relationship, Drug Discovery, medicine, Humans, 030304 developmental biology, media_common, 0303 health sciences, Molecular Structure, Chemistry, EV71, Tryptophan, virus diseases, HIV, Enterovirus a71, Virus Internalization, Antivirals, Virology, 0104 chemical sciences, 3. Good health, Enterovirus A, Human, 010404 medicinal & biomolecular chemistry, Viral replication, Indole, HIV-2, HIV-1, Molecular Medicine, Enterovirus, Capsid Proteins, Palladium-catalyzed C-H activation, Protein Binding
Abstract

Currently, there are only three FDA-approved drugs that inhibit human immunodeficiency virus (HIV) entry-fusion into host cells. The situation is even worse for enterovirus EV71 infection for which no antiviral therapies are available. We describe here the discovery of potent entry dual inhibitors of HIV and EV71. These compounds contain in their structure three or four tryptophan (Trp) residues linked to a central scaffold. Critical for anti-HIV/EV71 activity is the presence of extra phenyl rings, bearing one or two carboxylates, at the C2 position of the indole ring of each Trp residue. The most potent derivatives, 22 and 30, inhibit early steps of the replicative cycles of HIV-1 and EV-A71 by interacting with their respective viral surfaces (glycoprotein gp120 of HIV and the fivefold axis of the EV-A71 capsid). The high potency, low toxicity, facile chemical synthesis, and great opportunities for chemical optimization make them useful prototypes for future medicinal chemistry studies., This work was supported by the Spanish Plan Nacional (Subprograma Retos) [projects SAF2015-64629-C2-1-R and SAF2015-64629-C2-2-R (MINECO/FEDER)], the Spanish “Ministerio de Ciencia, Innovación y Universidades” (project PID2019-104070RB-C21), and by the Spanish Agencia Estatal Consejo Superior de Investigaciones Cientifí cas (CSIC, Projects CSIC-PIE-201980E100 and CSIC-PIE- 201980E028), “The Centers of Excellence” of the KU Leuven (EF-05/15 and PF-10/18), EU FP7 (FP7/2007−2013) Project EUVIRNA (Grant 408 Agreement 264286), EU FP7 SILVER (Contract HEALTH-F3-2010-260644), a grant from the Belgian Interuniversity Attraction Poles (IAP) Phase VIIP7/ 45 (BELVIR), and the EU FP7 Industry-Academia Partnerships and Pathways Project AIROPICO. The Spanish MEC/MINECO is also acknowledged for grants to B.M.-G. and O.M.-M. and the China Scholarship Council (CSC) (grant 201403250056) for a grant to L.S. S.H. received a grant from the Pennsylvania Department of Health using Tobacco CURE Funds. We also thank Charlotte Vanderheydt, Sandra Claes, and Evelyne Van Kerckhove for helping with the processing of the antiviral data. This work has been awarded with the Janssen (XVIII call) and Esteve (XIX call) prizes within the “Prizes for Young Researchers of the Spanish Society of Medicinal Chemistry (SEQT).

Published
2019

23. Filling Adeno-Associated Virus Capsids: Estimating Success by Cryo-Electron Microscopy

Author

Susan Hafenstein, Suriyasri Subramanian, James H. Marden, Luk H. Vandenberghe, James F. Conway, Anna C. Maurer, Turner Kevin, Alexander M. Makhov, and Carol M. Bator

Subjects
Cryo-electron microscopy, viruses, Genetic Vectors, Iterative reconstruction, Vectors in gene therapy, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Capsid, Microscopy, Genetics, medicine, Humans, Molecular Biology, Adeno-associated virus, Research Articles, 030304 developmental biology, Mathematics, 0303 health sciences, Cryoelectron Microscopy, Virion, Dependovirus, 030220 oncology & carcinogenesis, Cost analysis, Molecular Medicine, Capsid Proteins, Biological system
Abstract

Adeno-associated viruses (AAVs) have been employed successfully as gene therapy vectors in treating various genetic diseases for almost two decades. However, transgene packaging is usually imperfect, and developing a rapid and accurate method for measuring the proportion of DNA encapsidation is an important step for improving the downstream process of large scale vector production. In this study, we used two-dimensional class averages and three-dimensional classes, intermediate outputs in the single particle cryo-electron microscopy (cryo-EM) image reconstruction pipeline, to determine the proportion of DNA-packaged and empty capsid populations. Two different preparations of AAV3 were analyzed to estimate the minimum number of particles required to be sampled by cryo-EM in order for robust calculation of the proportion of the full versus empty capsids in any given sample. Cost analysis applied to the minimum amount of data required for a valid ratio suggests that cryo-EM is an effective approach to analyze vector preparations.

Published
2019

24. Examination and Reconstruction of Three Ancient Endogenous Parvovirus Capsid Protein Gene Remnants Found in Rodent Genomes

Author

Christian A. Urbina, Colin R. Parrish, Karen N. Barnard, Robert J. Gifford, Suriyasri Subramanian, Carol M. Bator, Robert A. Dick, Heather M. Callaway, and Susan Hafenstein

Subjects
Porcine parvovirus, Swine, Mus spretus, viruses, Immunology, Rodentia, Microbiology, Genome, Cell Line, Parvoviridae Infections, Parvovirus, Mice, 03 medical and health sciences, Capsid, Dogs, Virus-like particle, Virology, Sf9 Cells, Animals, Humans, Gene, 030304 developmental biology, Genetics, 0303 health sciences, biology, Structure and Assembly, 030302 biochemistry & molecular biology, Canine parvovirus, virus diseases, biology.organism_classification, Rats, HEK293 Cells, Insect Science, Cats, Capsid Proteins
Abstract

Parvovirus-derived endogenous viral elements (EVEs) have been found in the genomes of many different animal species, resulting from integration events that may have occurred from more than 50 million years ago to much more recently. Here, we further investigate the properties of autonomous parvovirus EVEs and describe their relationships to contemporary viruses. While we did not find any intact capsid protein open reading frames in the integrated viral sequences, we examined three EVEs that were repaired to form full-length sequences with relatively few changes. These sequences were found in the genomes of Rattus norvegicus (brown rat), Mus spretus (Algerian mouse), and Apodemus sylvaticus (wood mouse). The R. norvegicus sequence was not present in the genomes of the closely related species R. rattus, R. tanezumi, R. exulans, and R. everetti, indicating that it was less than 2 million years old, and the M. spretus and A. sylvaticus sequences were not found in the published genomes of other mouse species, also indicating relatively recent insertions. The M. spretus VP2 sequence assembled into capsids, which had high thermal stability, bound the sialic acid N-acetylneuraminic acid, and entered murine L cells. The 3.89-A structure of the M. spretus virus-like particles (VLPs), determined using cryo-electron microscopy, showed similarities to rodent and porcine parvovirus capsids. The repaired VP2 sequences from R. norvegicus and A. sylvaticus did not assemble as first prepared, but chimeras combining capsid surface loops from R. norvegicus with canine parvovirus assembled, allowing some of that capsid’s structures and functions to be examined. IMPORTANCE Parvovirus endogenous viral elements (EVEs) that have been incorporated into the genomes of different animals represent remnants of the DNA sequences of ancient viruses that infected the ancestors of those animals millions of years ago, but we know little about their properties or how they differ from currently circulating parvoviruses. By expressing the capsid proteins of different parvovirus EVEs that were found integrated into the genomes of three different rodents, we can examine their structures and functions. A VP2 (major capsid protein) EVE sequence from a mouse genome assembled into capsids that had a similar structure and biophysical properties to extant parvoviruses and also bound sialic acids and entered rodent cells. Chimeras formed from combinations of canine parvovirus and portions of the parvovirus sequences from the brown rat genome allowed us to examine the structures and functions of the surface loops of that EVE capsid.

Published
2019

25. Viral engagement with host receptors blocked by a novel class of tryptophan dendrimers that targets the 5-fold-axis of the enterovirus-A71 capsid

Author

Hyunwook Lee, Carol M. Bator, Pieter Leyssen, Johan Neyts, Kristina Lanko, Federico Gago, Hendrik Jan Thibaut, Carmen Mirabelli, Eva Rivero-Buceta, Ana San-Félix, Liang Sun, Kai Dallmeier, Belén Martínez-Gualda, Susan Hafenstein, Leen Delang, Ministerio de Economía y Competitividad (España), European Commission, Pennsylvania Department of Health, Belgian Science Policy Office, and China Scholarship Council

Subjects
Protein Conformation, viruses, Molecular Dynamics, Virus Replication, Viral Packaging, chemistry.chemical_compound, Binding Analysis, Protein structure, Computational Chemistry, Medicine and Health Sciences, Electron Microscopy, Biology (General), Internalization, Receptor, health care economics and organizations, media_common, Enterovirus, 0303 health sciences, Microscopy, Membrane Glycoproteins, 030302 biochemistry & molecular biology, Tryptophan, Drugs, Heparan sulfate, 3. Good health, Cell biology, Chemistry, Capsid, Physical Sciences, Research Article, Cell Binding, Cell Physiology, Dendrimers, QH301-705.5, media_common.quotation_subject, Immunology, Research and Analysis Methods, Microbiology, Antiviral Agents, Virus, 03 medical and health sciences, Virology, Microbial Control, Genetics, Enterovirus Infections, Humans, Molecular Biology, Chemical Characterization, 030304 developmental biology, Pharmacology, Heparin, Biology and Life Sciences, Electron Cryo-Microscopy, Cell Biology, RC581-607, Reverse genetics, Viral Replication, Viral replication, chemistry, Parasitology, Capsid Proteins, Antimicrobial Resistance, Heparitin Sulfate, Immunologic diseases. Allergy, HeLa Cells
Abstract

Enterovirus A71 (EV-A71) is a non-polio neurotropic enterovirus with pandemic potential. There are no antiviral agents approved to prevent or treat EV-A71 infections. We here report on the molecular mechanism by which a novel class of tryptophan dendrimers inhibits (at low nanomolar to high picomolar concentration) EV-A71 replication in vitro. A lead compound in the series (MADAL385) prevents binding and internalization of the virus but does not, unlike classical capsid binders, stabilize the particle. By means of resistance selection, reverse genetics and cryo-EM, we map the binding region of MADAL385 to the 5-fold vertex of the viral capsid and demonstrate that a single molecule binds to each vertex. By interacting with this region, MADAL385 prevents the interaction of the virus with its cellular receptors PSGL1 and heparan sulfate, thereby blocking the attachment of EV-A71 to the host cells., LS, KL, LD, PL, CM and JN received funding of Belgian Interuniversity Attraction Poles (IAP) Phase VII–P7/45 (BELVIR) and the EU FP7 Industry-Academia Partnerships and Pathways Project AIROPICO. LS received funding of China Scholarship Council (CSC) (Grant 201403250056). HL, CB and SH received a grant with the Pennsylvania Department of Health using Tobacco CURE Funds. ERB, BMG and ASF received the grant “Ministerio de Economia, Industriay Competitividad, Gobierno de España” and “European Regional Development Funds” projects number SAF2015-64629-C2-1-R (MINECO/ FEDER). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

Published
2019

27. Sample Preparation Induced Artifacts in Cryo-Electron Tomographs

Author

Dennis C. Winkler, Kaspars Tars, Carol M. Bator, Heather A. Holdaway, Michael G. Rossmann, Pavel Plevka, and Anthony J. Battisti

Subjects
Materials science, Cryo-electron microscopy, Icosahedral symmetry, Cryoelectron Microscopy, Cytological Techniques, Analytical chemistry, Electron, Article, Nuclear magnetic resonance, Viruses, Microscopy, Cathode ray, Bacteriophages, Sample preparation, Tomography, Artifacts, Instrumentation, Shrinkage
Abstract

We investigated the effects of sample preparation and of the exposure to an electron beam on particles in cryo-electron tomographs. Various virus particles with icosahedral symmetry were examined, allowing a comparison of symmetrically related components that should be identical in structure but might be affected differently by these imaging artifacts. Comparison of tomographic reconstructions with previously determined structures established by an independent method showed that neither freezing nor electron beam exposure produced a significant amount of shrinkage along the z axis (thickness). However, we observed damage to regions of the particles located close to the surface of the vitreous ice.

Published
2012

28. Interaction of Decay-Accelerating Factor with Coxsackievirus B3

Author

Carol M. Bator Kelly, Valorie D. Bowman, Paul R. Chipman, Michael G. Rossmann, M. Edward Medof, Feng Lin, and Susan Hafenstein

Subjects
Models, Molecular, viruses, Immunology, Picornaviridae, Virus Attachment, Plasma protein binding, Microbiology, Virology, Binding site, Receptor, Decay-accelerating factor, chemistry.chemical_classification, CD55 Antigens, biology, Cryoelectron Microscopy, fungi, virus diseases, Molecular biology, Virus-Cell Interactions, Enterovirus B, Human, Cell biology, chemistry, Membrane protein, Insect Science, biology.protein, Receptors, Virus, Antibody, Glycoprotein, Protein Binding
Abstract

Many entero-, parecho-, and rhinoviruses use immunoglobulin (Ig)-like receptors that bind into the viral canyon and are required to initiate viral uncoating during infection. However, some of these viruses use an alternative or additional receptor that binds outside the canyon. Both the coxsackievirus-adenovirus receptor (CAR), an Ig-like molecule that binds into the viral canyon, and decay-accelerating factor (DAF) have been identified as cellular receptors for coxsackievirus B3 (CVB3). A cryoelectron microscopy reconstruction of a variant of CVB3 complexed with DAF shows full occupancy of the DAF receptor in each of 60 binding sites. The DAF molecule bridges the canyon, blocking the CAR binding site and causing the two receptors to compete with one another. The binding site of DAF on CVB3 differs from the binding site of DAF on the surface of echoviruses, suggesting independent evolutionary processes.

Published
2007

29. Structure of decay-accelerating factor bound to echovirus 7: A virus-receptor complex

Author

Feng Lin, Menachem Shoham, Paul R. Chipman, Timothy S. Baker, M. Edward Medof, Richard J. Kuhn, Michael G. Rossmann, Yongning He, and Carol M. Bator

Subjects
Models, Molecular, Regulation of gene expression, Multidisciplinary, Echovirus, CD55 Antigens, viruses, Virus receptor, Cryoelectron Microscopy, fungi, Picornaviridae, virus diseases, Biological Sciences, Biology, medicine.disease_cause, Virology, Enterovirus B, Human, Protein Structure, Tertiary, Protein structure, medicine, Humans, Receptors, Virus, Enterovirus, Receptor, Decay-accelerating factor
Abstract

Echoviruses are enteroviruses that belong to Picornaviridae . Many echoviruses use decay-accelerating factor (DAF) as their cellular receptor. DAF is a glycosylphosphatidyl inositol-anchored complement regulatory protein found on most cell surfaces. It functions to protect cells from complement attack. The cryo-electron microscopy reconstructions of echovirus 7 complexed with DAF show that the DAF-binding regions are located close to the icosahedral twofold axes, in contrast to other enterovirus complexes where the viral canyon is the receptor binding site. This novel receptor binding position suggests that DAF is important for the attachment of viral particles to host cells, but probably not for initiating viral uncoating, as is the case with canyon-binding receptors. Thus, a different cell entry mechanism must be used for enteroviruses that bind DAF.

Published
2002

30. [Untitled]

Author

Carol M. Bator, Jason Howitt, Paul Freimuth, Paul R. Chipman, Yongning He, Timothy S. Baker, Carl W. Anderson, Richard J. Kuhn, Michael G. Rossmann, and Michael A. Whitt

Subjects
viruses, Virus receptor, virus diseases, Biology, Coxsackievirus, medicine.disease_cause, biology.organism_classification, Biochemistry, Molecular biology, Transmembrane protein, Cell biology, Adenoviridae, Transmembrane domain, Membrane protein, Structural Biology, Cytoplasm, Genetics, medicine, Receptor, human activities
Abstract

Group B coxsackieviruses (CVB) utilize the coxsackievirus-adenovirus receptor (CAR) to recognize host cells. CAR is a membrane protein with two Ig-like extracellular domains (D1 and D2), a transmembrane domain and a cytoplasmic domain. The three-dimensional structure of coxsackievirus B3 (CVB3) in complex with full length human CAR and also with the D1D2 fragment of CAR were determined to ∼22 A resolution using cryo-electron microscopy (cryo-EM). Pairs of transmembrane domains of CAR associate with each other in a detergent cloud that mimics a cellular plasma membrane. This is the first view of a virus–receptor interaction at this resolution that includes the transmembrane and cytoplasmic portion of the receptor. CAR binds with the distal end of domain D1 in the canyon of CVB3, similar to how other receptor molecules bind to entero- and rhinoviruses. The previously described interface of CAR with the adenovirus knob protein utilizes a side surface of D1.

Published
2001

31. Interaction of decay-accelerating factor with echovirus 7

Author

M. Edward Medof, Susan Hafenstein, Katharine G. Harris, Valorie D. Bowman, Javier O. Cifuente, Carol M. Bator, Pavel Plevka, Ying Zhang, Paul R. Chipman, Michael G. Rossmann, and Feng Lin

Subjects
Models, Molecular, Echovirus, Picornavirus, Protein Conformation, viruses, Immunology, Molecular Sequence Data, Picornaviridae, Echovirus Infections, Biology, medicine.disease_cause, Crystallography, X-Ray, Microbiology, Protein structure, Virology, medicine, Humans, Amino Acid Sequence, Binding site, Receptor, Peptide sequence, Decay-accelerating factor, Binding Sites, CD55 Antigens, Sequence Homology, Amino Acid, fungi, Cryoelectron Microscopy, virus diseases, biology.organism_classification, Enterovirus B, Human, Virus-Cell Interactions, Insect Science, Crystallization
Abstract

Echovirus 7 (EV7) belongs to the Enterovirus genus within the family Picornaviridae . Many picornaviruses use IgG-like receptors that bind in the viral canyon and are required to initiate viral uncoating during infection. However, in addition, some of the enteroviruses use an alternative or additional receptor that binds outside the canyon. Decay-accelerating factor (DAF) has been identified as a cellular receptor for EV7. The crystal structure of EV7 has been determined to 3.1-Å resolution and used to interpret the 7.2-Å-resolution cryo-electron microscopy reconstruction of EV7 complexed with DAF. Each DAF binding site on EV7 is near a 2-fold icosahedral symmetry axis, which differs from the binding site of DAF on the surface of coxsackievirus B3, indicating that there are independent evolutionary processes by which DAF was selected as a picornavirus accessory receptor. This suggests that there is an advantage for these viruses to recognize DAF during the initial process of infection.

Published
2010

32. Crystal structure of CD155 and electron microscopic studies of its complexes with polioviruses

Author

Valorie D. Bowman, Ping Zhang, Susan Hafenstein, Carol M. Bator, Eckard Wimmer, Marc C. Morais, Steffen Mueller, and Michael G. Rossmann

Subjects
Models, Molecular, Viral protein, Protein Conformation, viruses, Molecular Sequence Data, Biology, medicine.disease_cause, Crystallography, X-Ray, Virus, Cell Fusion, Protein structure, medicine, Humans, CD155, Amino Acid Sequence, Peptide sequence, Multidisciplinary, Cell fusion, Cryoelectron Microscopy, Biological Sciences, Molecular biology, Transmembrane protein, Poliovirus, Cytoplasm, Mutagenesis, biology.protein, Biophysics, Receptors, Virus, HeLa Cells
Abstract

When poliovirus (PV) recognizes its receptor, CD155, the virus changes from a 160S to a 135S particle before releasing its genome into the cytoplasm. CD155 is a transmembrane protein with 3 Ig-like extracellular domains, D1–D3, where D1 is recognized by the virus. The crystal structure of D1D2 has been determined to 3.5-Å resolution and fitted into ≈8.5-Å resolution cryoelectron microscopy reconstructions of the virus–receptor complexes for the 3 PV serotypes. These structures show that, compared with human rhinoviruses, the virus–receptor interactions for PVs have a greater dependence on hydrophobic interactions, as might be required for a virus that can inhabit environments of different pH. The pocket factor was shown to remain in the virus during the first recognition stage. The present structures, when combined with earlier mutational investigations, show that in the subsequent entry stage the receptor moves further into the canyon when at a physiological temperature, thereby expelling the pocket factor and separating the viral subunits to form 135S particles. These results provide a detailed analysis of how a nonenveloped virus can enter its host cell.

Published
2008

33. Structural and virological studies of the stages of virus replication that are affected by antirhinovirus compounds

Author

Tina M. Demenczuk, Adiba Watanyar, Daniel C. Pevear, Ying Zhang, Alan A. Simpson, Michael G. Rossmann, Carol M. Bator, Sugoto Chakravarty, Rebecca M. Ledford, and Gregory A. Skochko

Subjects
Models, Molecular, Rhinovirus, Viral protein, viruses, Immunology, Biology, medicine.disease_cause, Virus Replication, Microbiology, Antiviral Agents, Virus, chemistry.chemical_compound, X-Ray Diffraction, Virology, Vaccines and Antiviral Agents, medicine, Humans, Binding site, Oxazoles, Oxadiazoles, Binding Sites, Virus Assembly, RNA, Pleconaril, Viral replication, chemistry, Capsid, Insect Science, Crystallization, HeLa Cells
Abstract

Pleconaril is a broad-spectrum antirhinovirus and antienterovirus compound that binds into a hydrophobic pocket within viral protein 1, stabilizing the capsid and resulting in the inhibition of cell attachment and RNA uncoating. When crystals of human rhinovirus 16 (HRV16) and HRV14 are incubated with pleconaril, drug occupancy in the binding pocket is lower than when pleconaril is introduced during assembly prior to crystallization. This effect is far more marked in HRV16 than in HRV14 and is more marked with pleconaril than with other compounds. These observations are consistent with virus yield inhibition studies and radiolabeled drug binding studies showing that the antiviral effect of pleconaril against HRV16 is greater on the infectivity of progeny virions than the parent input viruses. These data suggest that drug integration into the binding pocket during assembly, or at some other late stage in virus replication, may contribute to the antiviral activity of capsid binding compounds.

Published
2004

34. Discrimination among rhinovirus serotypes for a variant ICAM-1 receptor molecule

Author

R. A. Killington, Tobias J. Tuthill, Carol M. Bator Kelly, Lisa J. Challinor, Paul R. Chipman, David J. Rowlands, Chuan Xiao, Alister Craig, and Michael G. Rossmann

Subjects
Models, Molecular, Virus genetics, Rhinovirus, Macromolecular Substances, Immunology, Molecular Sequence Data, Biology, In Vitro Techniques, medicine.disease_cause, Microbiology, Virus, Viral Proteins, Virology, medicine, Humans, Amino Acid Sequence, Binding site, Serotyping, Receptor, Peptide sequence, ICAM-1, Binding Sites, Sequence Homology, Amino Acid, Structure and Assembly, Genetic Variation, Intercellular Adhesion Molecule-1, Insect Science, Receptors, Virus, Salt bridge
Abstract

Intercellular adhesion molecule 1 (ICAM-1) is the cellular receptor for the major group of human rhinovirus serotypes, including human rhinovirus 14 (HRV14) and HRV16. A naturally occurring variant of ICAM-1, ICAM-1 Kilifi , has altered binding characteristics with respect to different HRV serotypes. HRV14 binds to ICAM-1 only transiently at physiological temperatures but forms a stable complex with ICAM-1 Kilifi . Conversely, HRV16 forms a stable complex with ICAM-1 but does not bind to ICAM-1 Kilifi . The three-dimensional structures of HRV14 and HRV16, complexed with ICAM-1, and the structure of HRV14, complexed with ICAM-1 Kilifi , have been determined by cryoelectron microscopy (cryoEM) image reconstruction to a resolution of approximately 10 Å. Structures determined by X-ray crystallography of both viruses and of ICAM-1 were fitted into the cryoEM density maps. The interfaces between the viruses and receptors contain extensive ionic networks. However, the interactions between the viruses and ICAM-1 Kilifi contain one less salt bridge than between the viruses and ICAM-1. As HRV16 has fewer overall interactions with ICAM-1 than HRV14, the absence of this charge interaction has a greater impact on the binding of ICAM-1 Kilifi to HRV16 than to HRV14.

Published
2004

35. Complexes of poliovirus serotypes with their common cellular receptor, CD155

Author

Eckard Wimmer, Valorie D. Bowman, Steffen Mueller, Suchetana Mukhopadhyay, Xiaozhong Peng, Michael G. Rossmann, Richard J. Kuhn, Yongning He, Carol M. Bator, and Paul R. Chipman

Subjects
Models, Molecular, Glycosylation, viruses, Immunology, Mutant, Molecular Sequence Data, medicine.disease_cause, Microbiology, Virus, Virology, medicine, Humans, CD155, Amino Acid Sequence, Binding site, Serotyping, Receptor, Peptide sequence, biology, Poliovirus, Virus receptor, Structure and Assembly, Cryoelectron Microscopy, Membrane Proteins, Molecular biology, Insect Science, biology.protein, Biophysics, Receptors, Virus
Abstract

Structures of all three poliovirus (PV) serotypes (PV1, PV2, and PV3) complexed with their cellular receptor, PV receptor (PVR or CD155), were determined by cryoelectron microscopy. Both glycosylated and fully deglycosylated CD155 exhibited similar binding sites and orientations in the viral canyon for all three PV serotypes, showing that all three serotypes use a common mechanism for cell entry. Difference maps between the glycosylated and deglycosylated CD155 complexes determined the sites of the carbohydrate moieties that, in turn, helped to verify the position of the receptor relative to the viral surface. The proximity of the CD155 carbohydrate site at Asn105 to the viral surface in the receptor-virus complex suggests that it might interfere with receptor docking, an observation consistent with the properties of mutant CD155. The footprints of CD155 on PV surfaces indicate that the south rim of the canyon dominates the virus-receptor interactions and may correspond to the initial CD155 binding state of the receptor-mediated viral uncoating. In contrast, the interaction of CD155 with the north rim of the canyon, especially the region immediately outside the viral hydrophobic pocket that normally binds a cellular “pocket factor,” may be critical for the release of the pocket factor, decreasing the virus stability and hence initiating uncoating. The large area of the CD155 footprint on the PV surface, in comparison with other picornavirus-receptor interactions, could be a potential limitation on the viability of PV escape mutants from antibody neutralization. Many of these are likely to have lost their ability to bind CD155, resulting in there being only three PV serotypes.

Published
2003

36. Interaction of Coxsackievirus A21 with Its Cellular Receptor, ICAM-1

Author

Elizabeth Rieder, Michael G. Rossmann, Valorie D. Bowman, Eckard Wimmer, Timothy S. Baker, Benoı̂t Hébert, Richard J. Kuhn, Jordi Bella, Carol M. Bator, Yongning He, and Chuan Xiao

Subjects
Models, Molecular, Protein Conformation, viruses, Immunology, Intercellular Adhesion Molecule-1, Coxsackievirus A21, Molecular Sequence Data, Biology, medicine.disease_cause, Microbiology, Protein structure, stomatognathic system, Virology, Extracellular, medicine, Image Processing, Computer-Assisted, Humans, Amino Acid Sequence, Binding site, Receptor, Peptide sequence, Enterovirus, Binding Sites, Poliovirus, Cryoelectron Microscopy, virus diseases, Virus-Cell Interactions, Protein Structure, Tertiary, Insect Science, Receptors, Virus
Abstract

Coxsackievirus A21 (CAV21), like human rhinoviruses (HRVs), is a causative agent of the common cold. It uses the same cellular receptor, intercellular adhesion molecule 1 (ICAM-1), as does the major group of HRVs; unlike HRVs, however, it is stable at acid pH. The cryoelectron microscopy (cryoEM) image reconstruction of CAV21 is consistent with the highly homologous crystal structure of poliovirus 1; like other enteroviruses and HRVs, CAV21 has a canyon-like depression around each of the 12 fivefold vertices. A cryoEM reconstruction of CAV21 complexed with ICAM-1 shows all five domains of the extracellular component of ICAM-1. The known atomic structure of the ICAM-1 amino-terminal domains D1 and D2 has been fitted into the cryoEM density of the complex. The site of ICAM-1 binding within the canyon of CAV21 overlaps the site of receptor recognition utilized by rhinoviruses and polioviruses. Interactions within this common region may be essential for triggering viral destabilization after attachment to susceptible cells.

Published
2001

37. Interaction of the poliovirus receptor with poliovirus

Author

Valorie D. Bowman, Xiaozhong Peng, Michael G. Rossmann, Yongning He, Jordi Bella, Carol M. Bator, Eckard Wimmer, Timothy S. Baker, Richard J. Kuhn, and Steffen Mueller

Subjects
Models, Molecular, Glycosylation, viruses, Sequence alignment, Biology, medicine.disease_cause, medicine, Image Processing, Computer-Assisted, Humans, CD155, Amino Acid Sequence, Receptor, Peptide sequence, chemistry.chemical_classification, Multidisciplinary, Virus receptor, Poliovirus, Cryoelectron Microscopy, Membrane Proteins, Biological Sciences, Molecular biology, chemistry, biology.protein, Biophysics, Receptors, Virus, Glycoprotein, Sequence Alignment, Poliovirus Receptor
Abstract

The structure of the extracellular, three-domain poliovirus receptor (CD155) complexed with poliovirus (serotype 1) has been determined to 22-Å resolution by means of cryo-electron microscopy and three-dimensional image-reconstruction techniques. Density corresponding to the receptor was isolated in a difference electron density map and fitted with known structures, homologous to those of the three individual CD155 Ig-like domains. The fit was confirmed by the location of carbohydrate moieties in the CD155 glycoprotein, the conserved properties of elbow angles in the structures of cell surface molecules with Ig-like folds, and the concordance with prior results of CD155 and poliovirus mutagenesis. CD155 binds in the poliovirus “canyon” and has a footprint similar to that of the intercellular adhesion molecule-1 receptor on human rhinoviruses. However, the orientation of the long, slender CD155 molecule relative to the poliovirus surface is quite different from the orientation of intercellular adhesion molecule-1 on rhinoviruses. In addition, the residues that provide specificity of recognition differ for the two receptors. The principal feature of receptor binding common to these two picornaviruses is the site in the canyon at which binding occurs. This site may be a trigger for initiation of the subsequent uncoating step required for viral infection.

Published
2000

38. Structural studies of two rhinovirus serotypes complexed with fragments of their cellular receptor

Author

Jordi Bella, Norman H. Olson, Timothy S. Baker, Prasanna R. Kolatkar, Michael G. Rossmann, and Carol M. Bator

Subjects
Models, Molecular, Molecular model, Rhinovirus, Cryo-electron microscopy, Molecular Sequence Data, Static Electricity, Biology, medicine.disease_cause, Crystallography, X-Ray, General Biochemistry, Genetics and Molecular Biology, Protein Structure, Secondary, medicine, Computer Graphics, Humans, Binding site, Serotyping, Cell adhesion, Receptor, Molecular Biology, ICAM-1, Binding Sites, General Immunology and Microbiology, General Neuroscience, Virus receptor, Cryoelectron Microscopy, Intercellular Adhesion Molecule-1, Virology, Biophysics, Receptors, Virus, Software, Research Article
Abstract

Two human rhinovirus serotypes complexed with two- and five-domain soluble fragments of the cellular receptor, intercellular adhesion molecule-1, have been investigated by X-ray crystallographic analyses of the individual components and by cryo-electron microscopy of the complexes. The three-dimensional image reconstructions provide a molecular envelope within which the crystal structures of the viruses and the receptor fragments can be positioned with accuracy. The N-terminal domain of the receptor binds to the rhinovirus 'canyon' surrounding the icosahedral 5-fold axes. Fitting of molecular models into the image reconstruction density identified the residues on the virus that interact with those on the receptor surface, demonstrating complementarity of the electrostatic patterns for the tip of the N-terminal receptor domain and the floor of the canyon. The complexes seen in the image reconstructions probably represent the first stage of a multistep binding process. A mechanism is proposed for the subsequent viral uncoating process.

Published
1999

39. Pseudo-atomic Structure of Coxsackievirus A21 Complexed with Its Cellular Receptor, ICAM-1

Author

Timothy S. Baker, Alister Craig, Carol M. Bator, Chuan Xiao, Michael G. Rossmann, Richard J. Kuhn, Paul R. Chipman, and Eckard Wimmer

Subjects
biology, Chemistry, viruses, Poliovirus, Coxsackievirus A21, virus diseases, RNA, Crystal structure, medicine.disease_cause, Virus, stomatognathic system, biology.protein, medicine, Biophysics, CD155, Receptor, Instrumentation, Peptide sequence
Abstract

Coxsackievirus A21 (CAV21), like human rhinoviruses (HRVs), is a causative agent of the common cold. CAV21 uses the same cellular receptor, intercellular adhesion molecule-1 (ICAM-1), as does the major group of HRVs. Moreover, unlike HRVs, CAV21 is stable over wide pH range. The CAV21 RNA genome has about 80% amino acid sequence identity to polioviruses (PVs), which utilize CD155 as their receptor. In contrast, CAV21 has only about 50% identity to HRVs. Interaction between the virus and the receptor had been studied by fitting atomic structure into a 26A resolution cryo-EM map. [1] However, the low resolution of the cryo-EM density limited the fitting accuracy and affected the interpretation of the interactions. Furthermore, the structure of CAV21, which had been fitted into the cryo-EM map, was modeled from the homologous structures of poliovirus 1 structure instead of using an X-ray crystallographic determined crystal structure.

Published
2002

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