Your search keyword '"Yellow fever virus pathogenicity"' showing total 19 results

1. Comparison of three neurotropic viruses reveals differences in viral dissemination to the central nervous system.

Author

Luethy LN, Erickson AK, Jesudhasan PR, Ikizler M, Dermody TS, and Pfeiffer JK

Subjects

Animals, Cell Line, Cricetinae, HeLa Cells, Humans, Interferon Type I immunology, Mice, Mice, Inbred C57BL, Mice, Knockout, Orthoreovirus, Mammalian growth & development, Poliomyelitis pathology, Poliomyelitis transmission, Poliovirus growth & development, Receptor, Interferon alpha-beta genetics, Reoviridae Infections pathology, Reoviridae Infections transmission, Sciatic Nerve virology, Yellow Fever pathology, Yellow Fever transmission, Yellow fever virus growth & development, Central Nervous System virology, Orthoreovirus, Mammalian pathogenicity, Peripheral Nerves virology, Poliovirus pathogenicity, Yellow fever virus pathogenicity

Abstract

Neurotropic viruses initiate infection in peripheral tissues prior to entry into the central nervous system (CNS). However, mechanisms of dissemination are not completely understood. We used genetically marked viruses to compare dissemination of poliovirus, yellow fever virus 17D (YFV-17D), and reovirus type 3 Dearing in mice from a hind limb intramuscular inoculation site to the sciatic nerve, spinal cord, and brain. While YFV-17D likely entered the CNS via blood, poliovirus and reovirus likely entered the CNS by transport through the sciatic nerve to the spinal cord. We found that dissemination was inefficient in adult immune-competent mice for all three viruses, particularly reovirus. Dissemination of all viruses was more efficient in immune-deficient mice. Although poliovirus and reovirus both accessed the CNS by transit through the sciatic nerve, stimulation of neuronal transport by muscle damage enhanced dissemination only of poliovirus. Our results suggest that these viruses access the CNS using different pathways., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2016

2. Historical Perspective: What Constitutes Discovery (of a New Virus)?

Author

Murphy FA

Subjects

Animals, Databases as Topic, Ebolavirus isolation & purification, Ebolavirus pathogenicity, Ebolavirus physiology, Encephalitis Virus, Murray Valley isolation & purification, Encephalitis Virus, Murray Valley pathogenicity, Encephalitis Virus, Murray Valley physiology, HIV-1 isolation & purification, HIV-1 pathogenicity, HIV-1 physiology, Hemorrhagic Fever Virus, Crimean-Congo isolation & purification, Hemorrhagic Fever Virus, Crimean-Congo pathogenicity, Hemorrhagic Fever Virus, Crimean-Congo physiology, History, 19th Century, History, 20th Century, Humans, Orthomyxoviridae isolation & purification, Orthomyxoviridae pathogenicity, Orthomyxoviridae physiology, Sin Nombre virus isolation & purification, Sin Nombre virus pathogenicity, Sin Nombre virus physiology, Ultrafiltration statistics & numerical data, Vaccinia virus isolation & purification, Vaccinia virus pathogenicity, Vaccinia virus physiology, Variola virus isolation & purification, Variola virus pathogenicity, Variola virus physiology, Workforce, Yellow fever virus isolation & purification, Yellow fever virus pathogenicity, Yellow fever virus physiology, Inventions history, Ultrafiltration history, Virology history

Abstract

A historic review of the discovery of new viruses leads to reminders of traditions that have evolved over 118 years. One such tradition gives credit for the discovery of a virus to the investigator(s) who not only carried out the seminal experiments but also correctly interpreted the findings (within the technological context of the day). Early on, ultrafiltration played a unique role in "proving" that an infectious agent was a virus, as did a failure to find any microscopically visible agent, failure to show replication of the agent in the absence of viable cells, thermolability of the agent, and demonstration of a specific immune response to the agent so as to rule out duplicates and close variants. More difficult was "proving" that the new virus was the etiologic agent of the disease ("proof of causation")-for good reasons this matter has been revisited several times over the years as technologies and perspectives have changed. One tradition is that the discoverers get to name their discovery, their new virus (unless some grievous convention has been broken)-the stability of these virus names has been a way to honor the discoverer(s) over the long term. Several vignettes have been chosen to illustrate several difficulties in holding to the traditions (vignettes chosen include vaccinia and variola viruses, yellow fever virus, and influenza viruses. Crimean-Congo hemorrhagic fever virus, Murray Valley encephalitis virus, human immunodeficiency virus 1, Sin Nombre virus, and Ebola virus). Each suggests lessons for the future. One way to assure that discoveries are forever linked with discoverers would be a permanent archive in one of the universal virus databases that have been constructed for other purposes. However, no current database seems ideal-perhaps members of the global community of virologists will have an ideal solution., (© 2016 Elsevier Inc. All rights reserved.)

Published

2016

3. Neurovirulence tests of three 17D yellow fever vaccine strains.

Author

Minor PD

Subjects

Animals, Antibodies, Neutralizing blood, Antibodies, Viral blood, Brain pathology, Macaca fascicularis, Mice, Spinal Cord pathology, Virulence immunology, Virus Cultivation, Yellow Fever immunology, Yellow Fever prevention & control, Yellow fever virus immunology, Yellow fever virus pathogenicity, Yellow Fever Vaccine toxicity

Abstract

The results of tests of the neurovirulence of three yellow fever vaccine preparations of different lineages are presented. Two preparations that have been used to make vaccines of acceptable safety and efficacy gave very similar results. A third preparation from the Robert Koch Institute, designated 168-73, was proposed as a reference preparation for the mouse potency assay in 1985 by WHO, but has been more often used as a reference in the monkey neurovirulence test. In the test described here 168-73 was of lower virulence than either of the other two preparations., (Copyright © 2011 The International Association for Biologicals. Published by Elsevier Ltd. All rights reserved.)

Published

2011

4. Differential cytokine responses from primary human Kupffer cells following infection with wild-type or vaccine strain yellow fever virus.

Author

Woodson SE, Freiberg AN, and Holbrook MR

Subjects

Adolescent, Cells, Cultured, Gene Expression Profiling, Humans, Male, Yellow fever virus pathogenicity, Cytokines metabolism, Kupffer Cells immunology, Kupffer Cells virology, Yellow fever virus immunology

Abstract

Wild-type yellow fever virus (YFV) infections result in a hepatotropic disease which is often fatal, while vaccination with the live-attenuated 17-D strain results in productive infection yet is well-tolerated with few adverse events. Kupffer cells (KCs) are resident liver macrophages that have a significant role in pathogen detection, clearance and immune signaling. Although KCs appear to be an important component of YF disease, their role has been under-studied. This study examined cytokine responses in KCs following infection with either wild-type or vaccine strains of YFV. Results indicate that KCs support replication of both wild-type and vaccine strains, yet wild-type YFV induced a prominent and prolonged pro-inflammatory cytokine response (IL-8, TNF-α and RANTES/CCL5) with little control by a major anti-inflammatory cytokine (IL-10). This response was significantly reduced in vaccine strain infections. These data suggest that a differentially regulated infection in KCs may play a critical role in development of disease., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

5. Efficient, trans-complementing packaging systems for chimeric, pseudoinfectious dengue 2/yellow fever viruses.

Author

Shustov AV and Frolov I

Subjects

Animals, Cell Line, Cricetinae, Defective Viruses genetics, Defective Viruses immunology, Defective Viruses pathogenicity, Defective Viruses physiology, Dengue Virus immunology, Dengue Virus pathogenicity, Genetic Complementation Test, Genome, Viral, Green Fluorescent Proteins genetics, Helper Viruses genetics, Helper Viruses physiology, Mutagenesis, Vaccines, Synthetic genetics, Viral Nonstructural Proteins genetics, Virus Replication, Yellow fever virus immunology, Yellow fever virus pathogenicity, Dengue Virus genetics, Dengue Virus physiology, Virus Assembly genetics, Virus Assembly physiology, Yellow fever virus genetics, Yellow fever virus physiology

Abstract

In our previous studies, we have stated to build a new strategy for developing defective, pseudoinfectious flaviviruses (PIVs) and applying them as a new type of vaccine candidates. PIVs combined the efficiency of live vaccines with the safety of inactivated or subunit vaccines. The results of the present work demonstrate further development of chimeric PIVs encoding dengue virus 2 (DEN2V) glycoproteins and yellow fever virus (YFV)-derived replicative machinery as potential vaccine candidates. The newly designed PIVs have synergistically functioning mutations in the prM and NS2A proteins, which abolish processing of the latter proteins and make the defective viruses capable of producing either only noninfectious, immature and/or subviral DEN2V particles. The PIV genomes can be packaged to high titers into infectious virions in vitro using the NS1-deficient YFV helper RNAs, and both PIVs and helpers can then be passaged as two-component genome viruses at an escalating scale., (Copyright 2010 Elsevier Inc. All rights reserved.)

Published

2010

6. A single M protein mutation affects the acid inactivation threshold and growth kinetics of a chimeric flavivirus.

Author

Maier CC, Delagrave S, Zhang ZX, Brown N, Monath TP, Pugachev KV, and Guirakhoo F

Subjects

Animals, Antiviral Agents pharmacology, Chlorocebus aethiops, Disease Models, Animal, Encephalitis Virus, Japanese drug effects, Encephalitis Virus, Japanese pathogenicity, Flavivirus Infections, Kinetics, Mice, Mutagenesis, Survival Analysis, Vero Cells, Viral Plaque Assay, Virulence, Virus Inactivation, Virus Replication, West Nile Virus Vaccines, Yellow fever virus drug effects, Yellow fever virus pathogenicity, Acids pharmacology, Amino Acid Substitution, Encephalitis Virus, Japanese genetics, Microbial Viability, Viral Matrix Proteins genetics, Yellow fever virus genetics

Abstract

Numerous viruses of the Flaviviridae family, including dengue, yellow fever, Japanese encephalitis, and West Nile, cause significant disease in humans and animals. The structure and function of the molecular components of the flavivirus envelope are therefore of significant interest. To our knowledge, a membrane (M) protein mutation which affects the pH at which flavivirus particles are inactivated in vitro has never been reported. Here we show that substitution of proline for glutamine at residue M5 (MQ5P) of a Japanese encephalitis-yellow fever chimera (ChimeriVax-JE) increases its acid sensitivity in vitro by 0.3 pH units (i.e., increases the pH at which virus titer is reduced by 50% from 6.08 to 6.38). In addition, growth kinetics of this mutant virus are accelerated in Vero cells, while neurovirulence and neuroinvasiveness measured in a mouse model are unaffected. A possible interpretation of these observations is that M can modulate the envelope (E) protein function during cell infection.

Published

2007

7. Yellow fever 17D virus: pseudo-revertant suppression of defective virus penetration and spread by mutations in domains II and III of the E protein.

Author

Vlaycheva L, Nickells M, Droll DA, and Chambers TJ

Subjects

Amino Acid Sequence, Animals, Chlorocebus aethiops, Defective Viruses genetics, Defective Viruses physiology, Models, Molecular, Molecular Sequence Data, Mutation, Vero Cells, Viral Envelope Proteins chemistry, Viral Envelope Proteins metabolism, Viral Plaque Assay, Yellow fever virus genetics, Yellow fever virus physiology, Defective Viruses pathogenicity, Suppression, Genetic, Viral Envelope Proteins genetics, Yellow fever virus pathogenicity

Abstract

A yellow fever (YFV) 17D virus variant, which causes persistent infection of mouse neuroblastoma cells associated with defective cell penetration and small plaque size, yielded plaque-revertant viruses from cells transfected with viral transcripts encoding the adaptive mutation (Gly360 in the E protein). Reconstruction of a plaque-purified revertant which contained Gly360 and additional substitutions (Asn for Lys303 and Val for Ala261) yielded a virus whose infectious center size, growth efficiency, and cell penetration rate similar to the parental YF5.2iv virus, whereas viruses with Asn303 or Val261 alone with Gly360 yielded either a small-plaque virus or a parental revertant. These data indicate that the YFV E protein is subject to suppression of mutations in domain III that are deleterious for viral entry and spread by a second-site mutation in domain II. Position 261 lies within the hydrophobic ligand-binding pocket at the domain I-II interface, a site believed to be involved in the hinge-like conformational change of domain II during activation of membrane fusion-activity. Results of this study provide genetic data consistent with findings on flavivirus structure and implicate domain III in functions beyond simply cell surface attachment.

Published

2004

8. Neurovirulence of yellow fever 17DD vaccine virus to rhesus monkeys.

Author

Marchevsky RS, Freire MS, Coutinho ES, and Galler R

Subjects

Animals, Antibodies, Viral blood, Central Nervous System pathology, Central Nervous System virology, Encephalitis, Viral prevention & control, Encephalitis, Viral virology, Female, Humans, Macaca mulatta, Male, Vaccines, Attenuated administration & dosage, Vaccines, Attenuated immunology, Viremia virology, Virulence, Yellow Fever physiopathology, Yellow Fever virology, Yellow Fever Vaccine administration & dosage, Yellow Fever Vaccine immunology, Yellow fever virus immunology, Encephalitis, Viral physiopathology, Vaccines, Attenuated adverse effects, Yellow Fever prevention & control, Yellow Fever Vaccine adverse effects, Yellow fever virus pathogenicity

Abstract

The yellow fever 17D virus is attenuated and used for human vaccination. Two of its substrains, 17D-204 and 17DD, are used for vaccine production. One of the remarkable properties of this vaccine is limited viral replication in the host but with significant dissemination of the viral mass, yielding a robust and long-lived neutralizing antibody response. The vaccine has excellent records of efficacy and safety and is cheap, used as a single dose, and there are well-established production methodology and quality control procedures which include the monkey neurovirulence test (MNTV). The present study aims at a better understanding of YF 17DD virus attenuation and immunogenicity in the MNVT with special emphasis on viremia, seroconversion, clinical and histological lesions scores, and their intrinsic variability across the tests. Several MNVTs were performed using the secondary seed lot virus 17DD 102/84 totaling 49 rhesus monkeys. Viremia was never higher than the accepted limits established in international requirements, and high levels of neutralizing antibodies were observed in all animals. None of the animals showed visceral lesions. We found that the clinical scores for the same virus varied widely across the tests. There was a direct correlation between the clinical scores in animals with clinical signs of encephalitis and a higher degree of central nervous system (CNS) histological lesions, with an increase of lesions in areas of the CNS such as the substantia nigra, nucleus caudatus, intumescentia cervicalis, and intumescentia ventralis. The histological scores were shown to be less prone to individual variations and had a more homogeneous value distribution among the tests. Since 17DD 102/84 seed virus has been used for human vaccine production and immunization for 16 years with the vaccine being safe and efficacious, it demonstrates that the observed variations across the MNVTs do not influence its effect on humans.

Published

2003

9. Pathogenesis and pathophysiology of yellow fever.

Author

Monath TP and Barrett AD

Subjects

Animals, Antibodies, Viral immunology, Disease Models, Animal, Disease Susceptibility, Humans, Liver pathology, Virulence, Yellow Fever immunology, Yellow Fever physiopathology, Yellow Fever Vaccine adverse effects, Yellow Fever Vaccine immunology, Yellow fever virus genetics, Yellow fever virus pathogenicity, Yellow Fever etiology

Abstract

It will be apparent to the reader that there is much to learn about the pathogenesis of YF. The role of specific genes and molecular determinants of neurotropism and viscerotropism has been defined only partially. The availability of infectious clones and a small animal (hamster) model should allow dissection of virulence factors, which can then be tested in the more difficult monkey model. The marked differences between wild-type YF strains should be evaluated by evaluating the relationships between virulence and genome sequence. The role of cytokine dysregulation and endothelial injury in YF will be elucidated as access to patients and of patients to more sophisticated medical care improves. The number of cases of YF in unvaccinated travelers hospitalized after return from the tropics has unfortunately increased, but such cases afford unique opportunities to study the pathogenesis of renal failure, coagulopathy, vascular instability, and shock, as well as new treatment modalities. At the cellular level, there are also important opportunities for research on YF virus-cell receptor interactions, the control of apoptotic cell death, and the predilection for cells of the midzone of the liver lobule. The role of dendritic cells in the early stage of YF infection is deserving of study. Finally, the role of the immune response to infection, particularly cellular immunity, is poorly characterized, and the suggestion that immune clearance may aggravate the condition of the host during the period of intoxication should be evaluated in appropriate animal models.

Published

2003

10. Heparan sulfate-mediated binding of infectious dengue virus type 2 and yellow fever virus.

Author

Germi R, Crance JM, Garin D, Guimet J, Lortat-Jacob H, Ruigrok RW, Zarski JP, and Drouet E

Subjects

Adsorption, Animals, CHO Cells, Chlorocebus aethiops, Cricetinae, Dengue virology, Vero Cells, Yellow Fever virology, Dengue Virus metabolism, Dengue Virus pathogenicity, Heparitin Sulfate metabolism, Yellow fever virus metabolism, Yellow fever virus pathogenicity

Abstract

Dengue virus type 2 and Yellow fever virus are arthropod-borne flaviviruses causing hemorrhagic fever in humans. Identification of virus receptors is important in understanding flavivirus pathogenesis. The aim of this work was to study the role of cellular heparan sulfate in the adsorption of infectious Yellow fever and Dengue type 2 viruses. Virus attachment was assessed by adsorbing virus to cells, washing unbound virus away, releasing cell-bound virus by freezing/thawing, and then titrating the released infectious virus. Treatment of cells by heparin-lyase, desulfation of cellular heparan sulfate, or treatment of the virus with heparin inhibited cell binding of both viruses. Heparin also inhibited Yellow fever virus infection by 97%. Using infectious virus, the present work shows the importance of heparan sulfate in binding and infection of these two flaviviruses.

Published

2002

11. In vitro potency assay for yellow fever vaccines: comparison of three vero cell lines sources.

Author

Fournier-Caruana J, Poirier B, Garnier F, and Fuchs F

Subjects

Animals, Chlorocebus aethiops, Consumer Product Safety, Quality Control, Vaccines, Attenuated, Vero Cells, Viral Plaque Assay, Viral Vaccines, Yellow fever virus pathogenicity

Abstract

Quality control of Yellow Fever vaccines performed by Control Authorities prior to marketing vaccines batches requires in vitro potency assays. The two currently available methods are the plaque formation assay and the cytopathic effect assay based on the use of porcine kidney PS cells or monkey kidney Vero cells. Among several sources of variation in virus titration, the cell systems are considered as important issues and Quality Assurance strongly recommends working with cell banks from certified suppliers. The aim of our study was to compare the behaviour and the sensitivity of three Vero cell sources obtained from ATCC, WHO and EP used at different passage levels in a plaque formation test. The conclusion of this work was that the yellow fever live attenuated virus titration, adapted in Vero cell lines appeared as a reliable method applicable for routine in vitro potency assay. The comparison of Vero cell lines, originated from three different sources, showed that they could be equally used as substrates by laboratories having the basic facility of cell culture, without influence on the final viral titre.

Published

2000

12. Mutagenesis of the RGD motif in the yellow fever virus 17D envelope protein.

Author

van der Most RG, Corver J, and Strauss JH

Subjects

Amino Acid Substitution, Animals, Cell Line, Cricetinae, Genetic Vectors, Models, Molecular, Mutagenesis, Sindbis Virus genetics, Transcription, Genetic, Transfection, Yellow fever virus genetics, Oligopeptides genetics, Viral Envelope Proteins genetics, Yellow fever virus pathogenicity

Abstract

The envelope protein of yellow fever virus 17D (YFV-17D) contains a solvent-exposed RGD motif, which has led to the suggestion that integrins may function as cellular receptors for YFV-17D. We found that mutating the RGD motif to RGE had no effect on viral titers, whereas changing RGD to TGD, TGE, TAD, TAE, or RGS led to reduced titers. Substitution of RGD by RAD or RAE yielded RNA genomes that replicated in mammalian cells but could not spread to neighboring cells at 37 degrees C. These mutants did spread through the cell monolayer at 30 degrees C (both in mosquito cells and in SW13 cells) and viruses grown at this temperature were capable of infecting mammalian cells at 37 degrees C. These results strongly suggest that RGD-mediated integrin binding does not play a major role in YFV-17D entry, since the RGD to RAD mutation, as well as many or all of the other mutations studied, should disrupt all RGD-dependent integrin binding. However, the RGD to RAD or RAE mutations (as well as TAD and TAE) severely destabilized the envelope protein at 37 degrees C, providing an explanation for the observed phenotype. Implications of these findings are discussed in light of the fact that mutations that alter tropism or virulence in different flaviviruses are often found within the loop containing the RGD motif., (Copyright 1999 Academic Press.)

Published

1999

13. Molecular and biological changes associated with HeLa cell attenuation of wild-type yellow fever virus.

Author

Dunster LM, Wang H, Ryman KD, Miller BR, Watowich SJ, Minor PD, and Barrett AD

Subjects

Animals, Humans, Mice, Species Specificity, Viral Envelope Proteins physiology, Virulence, Virus Replication, HeLa Cells virology, Yellow Fever virology, Yellow fever virus pathogenicity, Yellow fever virus physiology

Abstract

Six passages of the mosquito-borne flavivirus yellow fever (YF) wild-type strain Asibi in HeLa cells attenuated the virus for monkeys and newborn mice and resulted in loss of mosquito competence. Attenuation after the passage in HeLa cells was not unique to YF virus strain Asibi as demonstrated by the HeLa passage attenuation of wild-type YF virus strain French viscerotropic virus and YF vaccine virus 17D-204 for newborn mice. In contrast, wild-type strain Dakar 1279 and the French neurotropic vaccine virus remained virulent for newborn mice after six passages in HeLa cells. Thus not all strains of YF virus can be attenuated by passage in HeLa cells. Attenuation of YF virus strains Asibi and French viscerotropic virus was accompanied by alterations in the antigenic and biological properties of the viruses, including changes to envelope protein epitopes. Attenuation for newborn mice was coincidental with the acquisition by the HeLa-passaged viruses of the vaccine-specific envelope protein epitope recognized by monoclonal antibody H5. This suggests that this conformational change may play a role in the attenuation process. Wild-type Dakar 1279, which remained virulent for newborn mice after passage in HeLa cells, retained its wild-type antigenic character. The genome of Asibi HeLa p6 virus differed from wild-type Asibi virus by 29 nucleotides that encoded 10 amino acid substitutions: 5 in the envelope protein, 1 in NS2A, 3 in NS4B, and 1 in NS5. The substitution at NS4B-95 is seen in three different attenuation processes of wild-type YF virus, leading us to speculate that it is involved in the attenuation of virulence of wild-type strain Asibi.

Published

1999

14. Mutation in a 17D-204 vaccine substrain-specific envelope protein epitope alters the pathogenesis of yellow fever virus in mice.

Author

Ryman KD, Ledger TN, Campbell GA, Watowich SJ, and Barrett AD

Subjects

Animals, Brain pathology, Brain virology, Chlorocebus aethiops, Epitopes, B-Lymphocyte chemistry, Epitopes, B-Lymphocyte immunology, Female, Immunohistochemistry, Mice, Protein Conformation, Sequence Analysis, DNA, Vero Cells, Viral Envelope Proteins chemistry, Viral Envelope Proteins immunology, Virulence, Virus Replication, Yellow Fever pathology, Yellow Fever virology, Yellow fever virus immunology, Yellow fever virus physiology, Epitopes, B-Lymphocyte genetics, Point Mutation, Viral Envelope Proteins genetics, Viral Vaccines genetics, Viral Vaccines immunology, Yellow fever virus genetics, Yellow fever virus pathogenicity

Abstract

The heterogeneous nature of the yellow fever (YF) 17D-204 vaccine virus population was exploited in this study to isolate virus variants able to escape neutralization by the 17D-204 vaccine-specific MAb 864. The conformational change on the virus surface that resulted in the loss of the MAb 864-defined epitope was effected in each variant by a single amino acid mutation in the envelope (E) protein at either position E-305 or E-325. Interestingly, both positions were mutated during attenuation of the 17D-204 vaccine substrain from the wildtype Asibi strain. The mutations in several of the variants represented reversion to the wildtype Asibi virus sequence consistent with loss of a 17D-204 substrain-specific epitope. The majority of the variant viruses were shown to have altered mouse neurovirulence phenotypes, ranging from complete avirulence through to increased virulence. The avirulent variants are the first flavivirus MAb-neutralization-resistant variants to be attenuated for neurovirulence in the adult mouse model. Overall, the results indicate that the E protein epitope recognized by MAb 864 defines a functionally important region that encodes major molecular determinants of YF virus pathogenesis in vivo.

Published

1998

15. Antigenic variants of yellow fever virus with an altered neurovirulence phenotype in mice.

Author

Ryman KD, Xie H, Ledger TN, Campbell GA, and Barrett AD

Subjects

Animals, Brain pathology, Brain virology, Disease Models, Animal, Mice, Mice, Inbred C57BL, Phenotype, RNA, Viral analysis, Viral Envelope Proteins genetics, Virulence, Yellow Fever pathology, Yellow fever virus immunology, Antigenic Variation, Antigens, Viral genetics, Yellow Fever virology, Yellow fever virus genetics, Yellow fever virus pathogenicity

Abstract

The live-attenuated yellow fever (YF) vaccine virus, strain 17D-204, has long been known to consist of a heterologous population of virions. Gould et al. (J. Gen. Virol. 70, 1889-1894 (1989)) previously demonstrated that variant viruses exhibiting a YF wild-type-specific envelope (E) protein epitope are present at low frequency in the vaccine pool and were able to isolate representative virus variants with and without this epitope, designated 17D(+wt) and 17D(-wt), respectively. These variants were employed here in an investigation of YF virus pathogenesis in the mouse model. Both the 17D-204 parent and the 17D(+wt) variant viruses were lethal for adult outbred mice by the intracerebral route of inoculation. However, the 17D(-wt) variant was significantly attenuated (18% mortality rate) and replicated to much lower titer in the brains of infected mice. A single amino acid substitution in the envelope (E) protein at E-240 (Ala-->Val) was identified as responsible for the restricted replication of the 17D(-wt) variant in vivo. The 17D(+wt) variant has an additional second-site mutation, believed to encode a reversion to the neurovirulence phenotype of the 17D-204 parent virus. The amino acid substitution in the E protein at E-173 (Thr-->Ile) of the 17D(+wt) variant which results in the appearance of the wild-type-specific epitope or nucleotide changes in the 5' and 3' noncoding regions of the virus are proposed as a candidates.

Published

1997

16. Yellow fever vaccines.

Author

Barrett AD

Subjects

Animals, Cloning, Molecular, Humans, Vaccines, Attenuated, Yellow Fever prevention & control, Yellow fever virus genetics, Yellow fever virus pathogenicity, Viral Vaccines analysis, Viral Vaccines immunology, Yellow fever virus immunology

Published

1997

17. Mutagenesis of the N-linked glycosylation sites of the yellow fever virus NS1 protein: effects on virus replication and mouse neurovirulence.

Author

Muylaert IR, Chambers TJ, Galler R, and Rice CM

Subjects

Animals, Binding Sites, Brain Diseases virology, Cell Line, Cricetinae, Female, Flavivirus Infections virology, Glycosylation, Humans, Mice, Mice, Inbred ICR, Mutagenesis, Site-Directed, RNA, Viral metabolism, Transfection, Tumor Cells, Cultured, Viral Nonstructural Proteins physiology, Viral Proteins analysis, Virulence genetics, Virus Replication, Yellow fever virus genetics, Yellow fever virus physiology, Viral Nonstructural Proteins genetics, Yellow fever virus pathogenicity

Abstract

The flavivirus nonstructural glycoprotein NS1 is highly conserved and contains two N-linked glycosylation sites which are both utilized for addition of oligosaccharides during replication in cell culture. NS1 has been shown to contain epitopes for protective antibodies; however, its roles in virus replication and pathogenesis remain unknown. To study the function of NS1 during yellow fever virus replication, six mutant viruses which lack either one or both glycosylation sites and another one containing silent mutations at both sites were generated by site-directed mutagenesis. Mutants lacking the second glycosylation site and those bearing silent mutations were similar to the parental virus in their cell culture properties. Ablation of the first or both glycosylation sites generated mutants exhibiting small plaque phenotypes, decreased virus yields, reduced cytopathic effects, impaired NS1 secretion, and depressed RNA accumulation. In addition, mutants lacking the first or both glycosylation sites exhibited significant reduction in mouse neurovirulence after intracerebral inoculation. These defects appear to result from the lack of N-linked glycans rather than the introduction of deleterious amino acid substitutions or disruption of cis-acting RNA elements important for RNA replication. These results suggest an important role for NS1 in flavivirus RNA replication and pathogenesis.

Published

1996

18. Monoclonal antibodies distinguish between wild and vaccine strains of yellow fever virus by neutralization, hemagglutination inhibition, and immune precipitation of the virus envelope protein.

Author

Schlesinger JJ, Brandriss MW, and Monath TP

Subjects

Animals, Complement Fixation Tests, Epitopes, Hemagglutination Inhibition Tests, Hybridomas, Mice, Neutralization Tests, Precipitin Tests, Viral Envelope Proteins, Yellow fever virus pathogenicity, Antibodies, Monoclonal immunology, Antigens, Viral immunology, Viral Proteins immunology, Viral Vaccines, Yellow fever virus immunology

Abstract

Nineteen monoclonal antibodies were produced to the 17D strain of yellow fever virus (17D YF). Virus-specific structural and nonstructural proteins were identified for 17D YF and for the parent wild Asibi YF by radioimmunoprecipitation and sodium dodecyl sulfate-polyacrylamide gel electrophoresis. Fourteen of the monoclonal antibodies were directed against the envelope glycoprotein, E, and five against the nonstructural protein gp 48. The E protein of 17D YF was resolved as a double complex whereas the E protein of Asibi YF appeared as a single band of slightly lower molecular weight. The only IgM anti-E antibody obtained precipitated and neutralized 17D YF specifically with no activity against Asibi YF. This antibody also distinguished clearly by neutralization (N) between the 17D-204 derived vaccine strain to which the animal had been immunized and 17D YF strains of different origin. All 13 IgG anti-E monoclonal antibodies had hemagglutination-inhibition (HI) activity to 17D YF and all but one neutralized Asibi YF; however, only 3 of the 13 neutralized 17D YF. Four anti-E antibodies cross-reacted with other flaviviruses by HI or HI and N. Three of the five anti-gp 48 antibodies had complement-fixation (CF) titers against 17D YF and Asibi YF but none had N or HI activity.

Published

1983

19. A W.H.O. collaborative study of in vitro and in vivo methods for the assay of yellow fever vaccines.

Author

Seagroatt V and Magrath DI

Subjects

Animals, Cells, Cultured, Mice, Viral Plaque Assay, Viral Vaccines toxicity, World Health Organization, Yellow fever virus pathogenicity, Viral Vaccines immunology, Yellow fever virus immunology

Abstract

An international collaborative study was carried out to compare the plaque assay in monolayer cell cultures with the mouse assay for the potency testing of yellow fever vaccines. Twelve laboratories assayed four preparations of yellow fever virus by both methods. Differences were found between estimates of infectivities obtained by different laboratories using the plaque assay. There was also large variation between the estimates of mouse LD50 obtained by different laboratories. However, expressing potencies of the preparations relative to a common preparation greatly reduced the variation between laboratories for both the plaque and the mouse tests; it also resulted in remarkably close agreement between the methods.

Published

1983