Your search keyword '"Collins PL"' showing total 451 results

101. Experimental infection of adults with recombinant wild-type human metapneumovirus.

Author

Talaat KR, Karron RA, Thumar B, McMahon BA, Schmidt AC, Collins PL, and Buchholz UJ

Subjects

Adult, Animals, Antibodies, Neutralizing immunology, Antibodies, Viral blood, Antibodies, Viral immunology, Cytokines biosynthesis, Humans, Immunoglobulin A blood, Immunoglobulin A immunology, Immunoglobulin G blood, Immunoglobulin G immunology, Metapneumovirus genetics, Paramyxoviridae Infections prevention & control, Paramyxoviridae Infections virology, Respiratory Tract Infections immunology, Respiratory Tract Infections prevention & control, Respiratory Tract Infections virology, Vaccines, Attenuated administration & dosage, Vaccines, Attenuated immunology, Viral Load, Viral Vaccines administration & dosage, Viral Vaccines immunology, Virus Shedding, Metapneumovirus immunology, Paramyxoviridae Infections immunology

Abstract

Background: Human metapneumovirus (HMPV) causes lower respiratory tract infections in young children. rHMPV-SHs is a recombinant HMPV (rHMPV) based on a biologically derived wild-type HMPV strain. We characterized its infectivity and immunogenicity in healthy adults to determine whether it would be suitable for use as the parent virus for the development of live attenuated rHMPV vaccines., Methods: Twenty-one healthy adults were inoculated intranasally with 10(6) plaque-forming units of rHMPV-SHs. Respiratory symptoms and shedding of challenge virus were assessed. Neutralizing antibody responses, serum immunoglobulin G and A, and nasal wash specimen immunoglobulin A antibody responses to the HMPV F protein were also measured. Induction of nasal cytokines was assessed with electrochemiluminescence assays., Results: Nine subjects (43%) were infected with challenge virus as determined by virus detection and/or ≥4-fold rise in serum antibody titers. Peak viral shedding occurred on days 7-9 after infection. Four weeks after inoculation, 35% of subjects had any antibody response. Six of 9 infected subjects had respiratory symptoms, and 3 had headache after inoculation. Cytokine patterns differed considerably between subjects with similar illness severity and viral shedding., Conclusions: The rHMPV-SHs virus is infectious and is a suitable parent virus for development of live-attenuated HMPV vaccine candidates. Clinical Trials Registration. NCT01109329.

Published

2013

102. Evaluation of the replication, pathogenicity, and immunogenicity of avian paramyxovirus (APMV) serotypes 2, 3, 4, 5, 7, and 9 in rhesus macaques.

Author

Khattar SK, Nayak B, Kim SH, Xiao S, Samal S, Paldurai A, Buchholz UJ, Collins PL, and Samal SK

Subjects

Animals, Avulavirus classification, Avulavirus immunology, Chick Embryo, Chlorocebus aethiops, Macaca mulatta, Vero Cells, Avulavirus pathogenicity, Avulavirus Infections immunology

Abstract

Avian paramyxoviruses (APMV) serotypes 1-9 are frequently isolated from domestic and wild birds worldwide. APMV-1 (also called Newcastle disease virus, NDV) is attenuated in non-human primates and is being developed as a candidate human vaccine vector. The vector potential of the other serotypes was unknown. In the present study, we evaluated nine different biologically- or recombinantly-derived APMV strains for the ability to replicate and cause disease in rhesus macaque model. Five of the viruses were: biologically-derived wild type (wt) APMV-2, -3, -5, -7 and -9. Another virus was a recombinant (r) version of wt APMV-4. The remaining three viruses were versions of wt rAPMV-2, -4 and -7 in which the F cleavage site had been modified to be multi-basic. Rhesus macaques were inoculated intranasally and intratracheally and monitored for clinical disease, virus shedding from the upper and lower respiratory tract, and seroconversion. Virus shedding was not detected for wt APMV-5. Very limited shedding was detected for wt rAPMV-4 and modified rAPMV-4, and only in a subset of animals. Shedding by the other viruses was detected in every infected animal, and usually from both the upper and lower respiratory tract. In particular, shedding over a number of days in every animal was observed for modified rAPMV-2, wt APMV-7, and modified rAPMV-7. Modification of the F protein cleavage site appeared to increase shedding by wt rAPMV-2 and marginally by wt rAPMV-4. All APMVs except wt APMV-5 induced a virus-specific serum antibody response in all infected animals. None of the animals exhibited any clinical disease signs. These results indicate that APMVs 2, 3, 4, 7, and 9 are competent to infect non-human primates, but are moderately-to-highly restricted, depending on the serotype. This suggests that they are not likely to significantly infect primates in nature, and represent promising attenuated candidates for vector development.

Published

2013

103. Histone methylation keeps the brakes on autophagy.

Author

Collins PL and Oltz EM

Subjects

Animals, Humans, Autophagy genetics, Chromatin metabolism, Epigenesis, Genetic, Histocompatibility Antigens genetics, Histone-Lysine N-Methyltransferase genetics, T-Lymphocytes metabolism

Published

2013

104. Comparative immunogenicity of HIV-1 gp160, gp140 and gp120 expressed by live attenuated newcastle disease virus vector.

Author

Khattar SK, Samal S, LaBranche CC, Montefiori DC, Collins PL, and Samal SK

Subjects

AIDS Vaccines administration & dosage, Animals, Antibodies, Neutralizing biosynthesis, Antibodies, Neutralizing blood, Antibodies, Viral blood, Female, Gene Expression, Genetic Vectors, Guinea Pigs, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp160 genetics, HIV Infections blood, HIV Infections immunology, HIV Infections virology, Humans, Immunity, Humoral, Immunity, Mucosal, Mice, Mice, Inbred BALB C, Protein Engineering, Protein Structure, Tertiary, Recombinant Proteins genetics, Recombinant Proteins immunology, Vaccines, Attenuated, env Gene Products, Human Immunodeficiency Virus genetics, AIDS Vaccines immunology, Antibodies, Viral biosynthesis, HIV Envelope Protein gp120 immunology, HIV Envelope Protein gp160 immunology, HIV Infections prevention & control, HIV-1 immunology, Newcastle disease virus genetics, env Gene Products, Human Immunodeficiency Virus immunology

Abstract

The development of a vaccine against human immunodeficiency virus-1 (HIV-1) capable of inducing broad humoral and cellular responses at both the systemic and mucosal levels will be critical for combating the global AIDS epidemic. We previously demonstrated the ability of Newcastle disease virus (NDV) as a vaccine vector to express oligomeric Env protein gp160 and induce potent humoral and mucosal immune responses. In the present study, we used NDV vaccine strain LaSota as a vector to compare the biochemical and immunogenic properties of vector-expressed gp160, gp120, and two versions of gp140 (a derivative of gp160 made by deleting the transmembrane and cytoplasmic domains), namely: gp140L, which contained the complete membrane-proximal external region (MPER), and gp140S, which lacks the distal half of MPER. We show that, similar to gp160, NDV-expressed gp140S and gp120, but not gp140L, formed higher-order oligomers that retained recognition by conformationally sensitive monoclonal antibodies. Immunization of guinea pigs by the intranasal route with rLaSota/gp140S resulted in significantly greater systemic and mucosal antibody responses compared to the other recombinants. Immunization with rLaSota/140S, rLaSota/140L rLaSota/120 resulted in mixed Th1/Th2 immune responses as compared to Th1-biased immune responses induced by rLaSota/160. Importantly, rLaSota/gp140S induced neutralizing antibody responses to homologous HIV-1 strain BaL.26 and laboratory adapted HIV-1 strain MN.3 that were stronger than those elicited by the other NDV recombinants. Additionally, rLaSota/gp140S induced greater CD4+ and CD8+ T-cell responses in mice. These studies illustrate that rLaSota/gp140S is a promising vaccine candidate to elicit potent mucosal, humoral and cellular immune responses to the HIV-1 Env protein.

Published

2013

105. Mutations in the cytoplasmic domain of the Newcastle disease virus fusion protein confer hyperfusogenic phenotypes modulating viral replication and pathogenicity.

Author

Samal S, Khattar SK, Paldurai A, Palaniyandi S, Zhu X, Collins PL, and Samal SK

Subjects

Amino Acid Substitution, Animals, Cell Line, Humans, Mutant Proteins genetics, Mutant Proteins metabolism, Newcastle disease virus pathogenicity, Sequence Deletion, Viral Fusion Proteins genetics, Virulence, Newcastle disease virus physiology, Viral Fusion Proteins metabolism, Virus Replication

Abstract

The Newcastle disease virus (NDV) fusion protein (F) mediates fusion of viral and host cell membranes and is a major determinant of NDV pathogenicity. In the present study, we demonstrate the effects of functional properties of F cytoplasmic tail (CT) amino acids on virus replication and pathogenesis. Out of a series of C-terminal deletions in the CT, we were able to rescue mutant viruses lacking two or four residues (rΔ2 and rΔ4). We further rescued viral mutants with individual amino acid substitutions at each of these four terminal residues (rM553A, rK552A, rT551A, and rT550A). In addition, the NDV F CT has two conserved tyrosine residues (Y524 and Y527) and a dileucine motif (LL536-537). In other paramyxoviruses, these residues were shown to affect fusion activity and are central elements in basolateral targeting. The deletion of 2 and 4 CT amino acids and single tyrosine substitution resulted in hyperfusogenic phenotypes and increased viral replication and pathogenesis. We further found that in rY524A and rY527A viruses, disruption of the targeting signals did not reduce the expression on the apical or basolateral surface in polarized Madin-Darby canine kidney cells, whereas in double tyrosine mutant, it was reduced on both the apical and basolateral surfaces. Interestingly, in rL536A and rL537A mutants, the F protein expression was more on the apical than on the basolateral surface, and this effect was more pronounced in the rL537A mutant. We conclude that these wild-type residues in the NDV F CT have an effect on regulating F protein biological functions and thus modulating viral replication and pathogenesis.

Published

2013

106. The respiratory syncytial virus fusion protein and neutrophils mediate the airway mucin response to pathogenic respiratory syncytial virus infection.

Author

Stokes KL, Currier MG, Sakamoto K, Lee S, Collins PL, Plemper RK, and Moore ML

Subjects

Animals, Disease Models, Animal, Female, Humans, Infant, Lung pathology, Mice, Mice, Inbred BALB C, Respiratory Syncytial Virus Infections immunology, Respiratory Syncytial Virus Infections pathology, Respiratory Syncytial Virus Infections virology, Respiratory Syncytial Viruses isolation & purification, Viral Envelope Proteins metabolism, Viral Fusion Proteins immunology, Viral Load, Mucins metabolism, Neutrophils immunology, Respiratory Syncytial Viruses immunology, Respiratory Syncytial Viruses pathogenicity, Viral Fusion Proteins metabolism

Abstract

Respiratory syncytial virus (RSV) is the leading cause of death due to a viral etiology in infants. RSV disease is characterized by epithelial desquamation, neutrophilic bronchiolitis and pneumonia, and obstructive pulmonary mucus. It has been shown that infection of BALB/cJ mice with RSV clinical isolate A2001/2-20 (2-20) results in a higher early viral load, greater airway necrosis, and higher levels of interleukin-13 (IL-13) and airway mucin expression than infection with RSV laboratory strain A2. We hypothesized that the fusion (F) protein of RSV 2-20 is a mucus-inducing viral factor. In vitro, the fusion activity of 2-20 F but not that of A2 F was enhanced by expression of RSV G. We generated a recombinant F-chimeric RSV by replacing the F gene of A2 with the F gene of 2-20, generating A2-2-20F. Similar to the results obtained with the parent 2-20 strain, infection of BALB/cJ mice with A2-2-20F resulted in a higher early viral load and higher levels of subsequent pulmonary mucin expression than infection with the A2 strain. A2-2-20F infection induced greater necrotic airway damage and neutrophil infiltration than A2 infection. We hypothesized that the neutrophil response to A2-2-20F infection is involved in mucin expression. Antibody-mediated depletion of neutrophils in RSV-infected mice resulted in lower tumor necrosis factor alpha levels, fewer IL-13-expressing CD4 T cells, and less airway mucin production in the lung. Our data are consistent with a model in which the F and attachment (G) glycoprotein functional interaction leads to enhanced fusion and F is a key factor in airway epithelium infection, pathogenesis, and subsequent airway mucin expression.

Published

2013

107. Newcastle disease virus fusion protein is the major contributor to protective immunity of genotype-matched vaccine.

Author

Kim SH, Wanasen N, Paldurai A, Xiao S, Collins PL, and Samal SK

Subjects

Animals, Cell Line, Tumor, Chick Embryo, Chickens, Humans, Immunization, Newcastle Disease genetics, Newcastle Disease immunology, Newcastle Disease transmission, Mutation, Newcastle Disease prevention & control, Newcastle disease virus genetics, Newcastle disease virus immunology, Viral Fusion Proteins genetics, Viral Fusion Proteins immunology, Viral Vaccines genetics, Viral Vaccines immunology, Viral Vaccines pharmacology

Abstract

Virulent strains of Newcastle disease virus (NDV) can cause devastating disease in chickens worldwide. Although the current vaccines are substantially effective, they do not completely prevent infection, virus shedding and disease. To produce genotype-matched vaccines, a full-genome reverse genetics system has been used to generate a recombinant virus in which the F protein cleavage site has been changed to that of avirulent vaccine virus. In the other strategy, the vaccines have been generated by replacing the F and HN genes of a commercial vaccine strain with those from a genotype-matched virus. However, the protective efficacy of a chimeric virus vaccine has not been directly compared with that of a full-genome virus vaccine developed by reverse genetics. Therefore, in this study, we evaluated the protective efficacy of genotype VII matched chimeric vaccines by generating three recombinant viruses based on avirulent LaSota (genotype II) strain in which the open reading frames (ORFs) encoding the F and HN proteins were replaced, individually or together, with those of the circulating and highly virulent Indonesian NDV strain Ban/010. The cleavage site of the Ban/010 F protein was mutated to the avirulent motif found in strain LaSota. In vitro growth characteristics and a pathogenicity test indicated that all three chimeric viruses retained the highly attenuated phenotype of the parental viruses. Immunization of chickens with chimeric and full-length genome VII vaccines followed by challenge with virulent Ban/010 or Texas GB (genotype II) virus demonstrated protection against clinical disease and death. However, only those chickens immunized with chimeric rLaSota expressing the F or F plus HN proteins of the Indonesian strain were efficiently protected against shedding of Ban/010 virus. Our findings showed that genotype-matched vaccines can provide protection to chickens by efficiently preventing spread of virus, primarily due to the F protein.

Published

2013

108. Attenuation of live respiratory syncytial virus vaccines is associated with reductions in levels of nasal cytokines.

Author

Karron RA, Thumar B, Schappell E, Buchholz UJ, and Collins PL

Subjects

Biosensing Techniques, Female, Humans, Infant, Luminescent Measurements, Male, Nasal Mucosa chemistry, Respiratory Syncytial Virus Vaccines administration & dosage, Respiratory Syncytial Virus, Human pathogenicity, T-Lymphocytes, Regulatory immunology, Th1 Cells immunology, Th2 Cells immunology, Vaccines, Attenuated administration & dosage, Vaccines, Attenuated immunology, Cytokines metabolism, Nasal Mucosa immunology, Respiratory Syncytial Virus Vaccines immunology, Respiratory Syncytial Virus, Human immunology

Abstract

Background: Respiratory syncytial virus (RSV) is a leading cause of lower respiratory tract illness (LRTI) in children. Several promising live-attenuated RSV vaccines are in development. Defining additional markers of attenuation could enhance clinical trials., Methods: We used clinical data, virologic data, and nasal wash (NW) specimens from 20 RSV-naive children enrolled in studies of 4 live-attenuated RSV vaccines. Seven received minimally attenuated cpts248/955 or cpts530/1009 (group 1), 6 received moderately attenuated cpts248/404 (group 2), and 7 received highly attenuated rA2cp248/404/1030/ΔSH (group 3). NW specimens were tested for cytokines and chemokines via an electrochemiluminescence biosensor assay., Results: Group 1 exhibited 1 instance of LRTI and significantly higher rates of fever than groups 2 or 3; there were no significant differences in peak titers of vaccine virus in NW specimens. In contrast, levels of interferon γ, interleukin 1β, interleukin 2, interleukin 6, and interleukin 13 were significantly greater in NW specimens from group 1, compared with those from group 3. Maximum increases in levels of most cytokines occurred after peak viral replication but coincided with clinical illness., Conclusions: Substantial increases in proinflammatory, antiinflammatory, T-helper 1, T-helper 2, and regulatory cytokines were detected in children who received minimally attenuated live RSV vaccines but not in children who received highly attenuated vaccines. Levels of cytokines in NW specimens may be useful biomarkers of attenuation for live RSV vaccines.

Published

2013

109. Epigenetic Activation and Silencing of the Gene that Encodes IFN-γ.

Author

Aune TM, Collins PL, Collier SP, Henderson MA, and Chang S

Abstract

Transcriptional activation and repression of genes that are developmentally regulated or exhibit cell-type specific expression patterns is largely achieved by modifying the chromatin template at a gene locus. Complex formation of stable epigenetic histone marks, loss or gain of DNA methylation, alterations in chromosome conformation, and specific utilization of both proximal and distal transcriptional enhancers and repressors all contribute to this process. In addition, long non-coding RNAs are a new species of regulatory RNAs that either positively or negatively regulate transcription of target gene loci. IFN-γ is a pro-inflammatory cytokine with critical functions in both innate and adaptive arms of the immune system. This review focuses on our current understanding of how the chromatin template is modified at the IFNG locus during developmental processes leading to its transcriptional activation and silencing.

Published

2013

110. Control of Ig gene assembly: lessons from premature activation.

Author

Gopalakrishnan S, Collins PL, and Oltz EM

Subjects

Animals, Histones metabolism, Interferon Regulatory Factors metabolism, Precursor Cells, B-Lymphoid physiology, V(D)J Recombination physiology

Published

2013

111. Neonatal antibody responses are attenuated by interferon-γ produced by NK and T cells during RSV infection.

Author

Tregoning JS, Wang BL, McDonald JU, Yamaguchi Y, Harker JA, Goritzka M, Johansson C, Bukreyev A, Collins PL, and Openshaw PJ

Subjects

Analysis of Variance, Animals, Enzyme-Linked Immunosorbent Assay, Female, Flow Cytometry, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Pregnancy, Animals, Newborn, Antibodies, Viral immunology, Interferon-gamma immunology, Killer Cells, Natural immunology, Respiratory Syncytial Virus Infections immunology, T-Lymphocytes immunology

Abstract

Respiratory syncytial virus (RSV) infects most children in the first year of life and is a major single cause of hospitalization in infants and young children. There is no effective vaccine, and antibody generated by primary neonatal infection is poorly protective against reinfection even with antigenically homologous viral strains. Studying the immunological basis of these observations in neonatal mice, we found that antibody responses to infection were low and unaffected by CD4 depletion, in contrast with adult mice, which had stronger CD4-dependent antibody responses. Natural killer cell depletion or codepletion of CD4(+) and CD8(+) cells during neonatal RSV infection caused a striking increase in anti-RSV antibody titer. These cells are major sources of the cytokine IFN-γ, and blocking IFN-γ also enhanced RSV-specific antibody responses in neonates. In addition, infection with a recombinant RSV engineered to produce IFN-γ reduced antibody titer, confirming that IFN-γ plays a pivotal role in inhibition of antibody responses after neonatal infection. These unexpected findings show that the induction of a strong cellular immune response may limit antibody responses in early life and that vaccines that induce IFN-γ-secreting cells might, in some situations, be less protective than those that do not.

Published

2013

112. Phylogenetic and pathotypic characterization of newcastle disease viruses circulating in west Africa and efficacy of a current vaccine.

Author

Samuel A, Nayak B, Paldurai A, Xiao S, Aplogan GL, Awoume KA, Webby RJ, Ducatez MF, Collins PL, and Samal SK

Subjects

Animals, Benin epidemiology, Chickens, Cluster Analysis, Genotype, Molecular Sequence Data, Newcastle Disease epidemiology, Newcastle disease virus genetics, Newcastle disease virus isolation & purification, Phylogeny, Sequence Analysis, DNA, Survival Analysis, Togo epidemiology, Viral Vaccines administration & dosage, Virulence, Virus Shedding, Genetic Variation, Newcastle Disease prevention & control, Newcastle Disease virology, Newcastle disease virus classification, Newcastle disease virus pathogenicity, Viral Vaccines immunology

Abstract

Newcastle disease (ND) is a deadly avian disease worldwide. In Africa, ND is enzootic and causes large economic losses, but little is known about the Newcastle disease virus (NDV) strains circulating in African countries. In this study, 27 NDV isolates collected from apparently healthy chickens in live-bird markets of the West African countries Benin and Togo in 2009 were characterized. All isolates had polybasic fusion (F)-protein cleavage sites and were shown to be highly virulent in standard pathogenicity assays. Infection of 2-week-old chickens with two of the isolates resulted in 100% mortality within 4 days. Phylogenetic analysis of the 27 isolates based on a partial F-protein gene sequence identified three clusters: one containing all the isolates from Togo and one from Benin (cluster 2), one containing most isolates from Benin (cluster 3), and an outlier isolate from Benin (cluster 1). All the three clusters are related to genotype VII strains of NDV. In addition, the cluster of viruses from Togo contained a recently identified 6-nucleotide insert between the hemagglutinin-neuraminidase (HN) and large polymerase (L) genes in a complete genome of an NDV isolate from this geographical region. Multiple strains that include this novel element suggest local emergence of a new genome length class. These results reveal genetic diversity within and among local NDV populations in Africa. Sequence analysis showed that the F and HN proteins of six West African isolates share 83.2 to 86.6% and 86.5 to 87.9% identities, respectively, with vaccine strain LaSota, indicative of considerable diversity. A vaccine efficacy study showed that the LaSota vaccine protected birds from morbidity and mortality but did not prevent shedding of West African challenge viruses.

Published

2013

113. Respiratory syncytial virus modified by deletions of the NS2 gene and amino acid S1313 of the L polymerase protein is a temperature-sensitive, live-attenuated vaccine candidate that is phenotypically stable at physiological temperature.

Author

Luongo C, Winter CC, Collins PL, and Buchholz UJ

Subjects

Animals, Disease Models, Animal, Female, Humans, Mice, Mice, Inbred BALB C, Pan troglodytes, Respiratory Syncytial Virus Infections pathology, Respiratory Syncytial Virus Infections virology, Respiratory Syncytial Virus Vaccines genetics, Respiratory Syncytial Virus, Human genetics, Respiratory Syncytial Virus, Human pathogenicity, Respiratory Tract Infections pathology, Respiratory Tract Infections virology, Temperature, Vaccines, Attenuated genetics, Vaccines, Attenuated immunology, Virulence, Gene Deletion, Mutation, Missense, Respiratory Syncytial Virus Vaccines immunology, Respiratory Syncytial Virus, Human growth & development, Respiratory Syncytial Virus, Human immunology, Viral Proteins genetics

Abstract

Human respiratory syncytial virus (RSV) is the leading viral cause of lower respiratory tract disease in infants and children worldwide. In previous work to develop point mutations in RSV with improved genetic stability, we observed that an attenuating mutation at amino acid position 1321 in the L polymerase protein was subject to deattenuation by a spontaneous second-site compensatory mutation at position 1313 (C. Luongo, C. C. Winter, P. L. Collins, and U. J. Buchholz, J. Virol. 86:10792-10804, 2012). In the present study, we found that deletion of position 1313 (Δ1313), irrespective of the presence of an attenuating mutation at position 1321, provided a new attenuating mutation. RSV bearing Δ1313 replicated in cell culture as efficiently as wild-type virus at 32°C, was restricted for replication at 37°C, and was restricted 50-fold and 150-fold in the upper and lower respiratory tracts, respectively, of mice. We combined the Δ1313 deletion with the previously described, attenuating NS2 gene deletion (ΔNS2) to produce the recombinant live-attenuated RSV vaccine candidate ΔNS2/Δ1313. During in vitro stress tests involving serial passage at incrementally increasing temperatures, a second-site compensatory mutation was detected in close proximity of Δ1313, namely, I1314T. This site was genetically and phenotypically stabilized by an I1314L substitution. Combination of I1314L with ΔNS2/Δ1313 yielded a virus, ΔNS2/Δ1313/1314L, with genetic stability at physiological temperature. This stabilized vaccine candidate was moderately temperature sensitive and had a level of restriction in chimpanzees comparable to that of MEDI-559, a promising RSV vaccine candidate that presently is in clinical trials but lacks stabilized attenuating mutations. The level of attenuation and genetic stability identify ΔNS2/Δ1313/1314L as a promising candidate for evaluation in pediatric phase I studies.

Published

2013

114. p38 and OGT sequestration into viral inclusion bodies in cells infected with human respiratory syncytial virus suppresses MK2 activities and stress granule assembly.

Author

Fricke J, Koo LY, Brown CR, and Collins PL

Subjects

Cell Line, Epithelial Cells chemistry, Epithelial Cells virology, Humans, Protein Transport, Signal Transduction, Inclusion Bodies, Viral metabolism, Intracellular Signaling Peptides and Proteins antagonists & inhibitors, Intracellular Signaling Peptides and Proteins metabolism, N-Acetylglucosaminyltransferases metabolism, Protein Serine-Threonine Kinases antagonists & inhibitors, Protein Serine-Threonine Kinases metabolism, Respiratory Syncytial Virus, Human pathogenicity, p38 Mitogen-Activated Protein Kinases metabolism

Abstract

Respiratory syncytial virus (RSV) forms cytoplasmic inclusion bodies (IBs) that are thought to be sites of nucleocapsid accumulation and viral RNA synthesis. The present study found that IBs also were the sites of major sequestration of two proteins involved in cellular signaling pathways. These are phosphorylated p38 mitogen-activated protein kinase (MAPK) (p38-P), a key regulator of cellular inflammatory and stress responses, and O-linked N-acetylglucosamine (OGN) transferase (OGT), an enzyme that catalyzes the posttranslational addition of OGN to protein targets to regulate cellular processes, including signal transduction, transcription, translation, and the stress response. The virus-induced sequestration of p38-P in IBs resulted in a substantial reduction in the accumulation of a downstream signaling substrate, MAPK-activated protein kinase 2 (MK2). Sequestration of OGT in IBs was associated with suppression of stress granule (SG) formation. Thus, while the RSV IBs are thought to play an essential role in viral replication, the present results show that they also play a role in suppressing the cellular response to viral infection. The sequestration of p38-P and OGT in IBs appeared to be reversible: oxidative stress resulting from arsenite treatment transformed large IBs into a scattering of smaller bodies, suggestive of partial disassembly, and this was associated with MK2 phosphorylation and OGN addition. Unexpectedly, the RSV M2-1 protein was found to localize in SGs that formed during oxidative stress. This protein was previously shown to be a viral transcription elongation factor, and the present findings provide the first evidence of possible involvement in SG activities during RSV infection.

Published

2013

115. Complete genome sequence of a highly virulent newcastle disease virus currently circulating in Mexico.

Author

Xiao S, Paldurai A, Nayak B, Mirande A, Collins PL, and Samal SK

Abstract

The complete genome sequence was determined for a highly virulent Newcastle disease virus strain from vaccinated chicken farms in Mexico during outbreaks in 2010. On the basis of phylogenetic analysis this strain was classified into genotype V in the class II cluster that was closely related to Mexican strains that appeared in 2004-2006.

Published

2013

116. Complete genome sequence of an avian paramyxovirus type 4 from north america reveals a shorter genome and new genotype.

Author

Parthiban M, Kaliyaperumal M, Xiao S, Nayak B, Paldurai A, Kim SH, Ladman BS, Preskenis LA, Gelb J Jr, Collins PL, and Samal SK

Abstract

An avian paramyxovirus type 4 (APMV-4) was isolated from a duck in Delaware in 2010. Its genome is 15,048 nucleotides (nt) long, which is shorter by 6 nt than those for all previously reported strains. Phylogenetic analysis revealed that this strain formed a separate cluster within APMV-4 strains.

Published

2013

117. Mutations in the fusion protein cleavage site of avian paramyxovirus serotype 4 confer increased replication and syncytium formation in vitro but not increased replication and pathogenicity in chickens and ducks.

Author

Kim SH, Xiao S, Shive H, Collins PL, and Samal SK

Subjects

Amino Acid Sequence, Animals, Antibodies, Viral immunology, Avulavirus classification, Avulavirus genetics, Avulavirus immunology, Avulavirus Infections veterinary, Avulavirus Infections virology, Base Sequence, Brain pathology, Brain virology, Cell Line, Cytopathogenic Effect, Viral, Humans, Immunohistochemistry, Kinetics, Molecular Sequence Data, Mutant Proteins metabolism, Neurons pathology, Neurons virology, Proteolysis, Reverse Genetics, Serotyping, Viral Fusion Proteins chemistry, Virion metabolism, Avulavirus pathogenicity, Chickens virology, Ducks virology, Giant Cells virology, Mutation genetics, Viral Fusion Proteins genetics, Virus Replication genetics

Abstract

To evaluate the role of the F protein cleavage site in the replication and pathogenicity of avian paramyxoviruses (APMVs), we constructed a reverse genetics system for recovery of infectious recombinant APMV-4 from cloned cDNA. The recovered recombinant APMV-4 resembled the biological virus in growth characteristics in vitro and in pathogenicity in vivo. The F cleavage site sequence of APMV-4 (DIQPR↓F) contains a single basic amino acid, at the -1 position. Six mutant APMV-4 viruses were recovered in which the F protein cleavage site was mutated to contain increased numbers of basic amino acids or to mimic the naturally occurring cleavage sites of several paramyxoviruses, including neurovirulent and avirulent strains of NDV. The presence of a glutamine residue at the -3 position was found to be important for mutant virus recovery. In addition, cleavage sites containing the furin protease motif conferred increased replication and syncytium formation in vitro. However, analysis of viral pathogenicity in 9-day-old embryonated chicken eggs, 1-day-old and 2-week-old chickens, and 3-week-old ducks showed that none the F protein cleavage site mutations altered the replication, tropism, and pathogenicity of APMV-4, and no significant differences were observed among the parental and mutant APMV-4 viruses in vivo. Although parental and mutant viruses replicated somewhat better in ducks than in chickens, they all were highly restricted and avirulent in both species. These results suggested that the cleavage site sequence of the F protein is not a limiting determinant of APMV-4 pathogenicity in chickens and ducks.

Published

2013

118. Live-attenuated respiratory syncytial virus vaccines.

Author

Karron RA, Buchholz UJ, and Collins PL

Subjects

Administration, Intranasal, Antibodies, Viral biosynthesis, Child, Preschool, Genetic Vectors chemistry, Genetic Vectors immunology, Humans, Immunity, Cellular drug effects, Immunity, Humoral drug effects, Immunity, Innate drug effects, Infant, Respiratory Syncytial Virus Infections pathology, Respiratory Syncytial Virus Infections virology, Respiratory Syncytial Virus Vaccines administration & dosage, Respiratory Syncytial Virus, Human pathogenicity, Respirovirus genetics, Respirovirus immunology, Reverse Genetics methods, Vaccines, Attenuated, Antibodies, Viral immunology, Respiratory Syncytial Virus Infections immunology, Respiratory Syncytial Virus Infections prevention & control, Respiratory Syncytial Virus Vaccines immunology, Respiratory Syncytial Virus, Human immunology

Abstract

Live-attenuated respiratory syncytial virus (RSV) vaccines offer several advantages for immunization of infants and young children: (1) they do not cause vaccine-associated enhanced RSV disease; (2) they broadly stimulate innate, humoral, and cellular immunity, both systemically and locally in the respiratory tract; (3) they are delivered intranasally; and (4) they replicate in the upper respiratory tract of young infants despite the presence of passively acquired maternally derived RSV neutralizing antibody. This chapter describes early efforts to develop vaccines through the classic methods of serial cold-passage and chemical mutagenesis, and recent efforts using reverse genetics to derive attenuated derivatives of wild-type (WT) RSV and to develop parainfluenza vaccine vectors that express RSV surface glycoproteins.

Published

2013

119. Evaluation of the genetic diversity of avian paramyxovirus type 4.

Author

Nayak B, Nayak S, Paldurai A, Kumar S, De Nardi R, Terregino C, Collins PL, and Samal SK

Subjects

Animals, Avulavirus growth & development, Base Sequence, Cell Line, Chick Embryo, Chickens, Gene Order, Genome, Viral, Molecular Sequence Data, Phosphoproteins chemistry, Phosphoproteins genetics, Phylogeny, Sequence Alignment, Sequence Analysis, DNA, Serotyping, Viral Proteins chemistry, Viral Proteins genetics, Avulavirus classification, Avulavirus genetics, Genetic Variation

Abstract

Avian paramyxoviruses (APMVs) belong to the genus Avulavirus in the family Paramyxoviridae and include at least nine serotypes, APMV-1 to -9, as well as two additional provisional serotypes. Newcastle disease virus (NDV), which comprises APMV-1, is the most extensively studied APMV because it is an important poultry pathogen. A moderate level of antigenic and genetic diversity is recognized for APMV-1 isolates, but our knowledge of the antigenic and genetic diversity of the other APMV serotypes is limited. APMV-4 is frequently isolated from waterfowl around the world. To date complete genome sequences of APMV-4 are available for only strains, which were isolated from ducks in Hong Kong, Korea and Belgium over a period of 37 years. We have carried out genome sequencing from the nucleocapsid (N) gene-end signal to the polymerase (L) gene-start signal of five APMV-4 strains recently isolated from Italy. Each of the eight APMV-4 strains has the same F protein cleavage site, DIQPR↓F. They also share a high level of nucleotide and amino acid sequence identity: for example, the F and HN glycoproteins have greater than 97% sequence identity between the various strains. Thus, comparison of these eight strains of APMV-4 did not provide evidence of substantial diversity, in contrast to similar studies with APMV-2, -3, and -6, in which the F and HN glycoproteins exhibited up to 20-30% amino acid sequence variation within a subgroup. Reciprocal cross-HI assay using post infection chicken sera also failed to detect significant antigenic variation among the available APMV-4 strains., (Published by Elsevier B.V.)

Published

2013

120. Respiratory syncytial virus: virology, reverse genetics, and pathogenesis of disease.

Author

Collins PL, Fearns R, and Graham BS

Subjects

Base Sequence, Host Specificity, Humans, Molecular Sequence Data, Respiratory Syncytial Virus Infections physiopathology, Respiratory Syncytial Virus Infections virology, Respiratory Syncytial Virus Vaccines administration & dosage, Respiratory Syncytial Virus Vaccines adverse effects, Respiratory Syncytial Virus, Human immunology, Respiratory Syncytial Virus, Human pathogenicity, Reverse Genetics, Vaccines, Attenuated, Viral Proteins immunology, Viral Tropism, Virus Replication, Gene Expression Regulation, Viral, Genes, Viral, Genome, Viral, Respiratory Syncytial Virus Infections prevention & control, Respiratory Syncytial Virus Vaccines immunology, Respiratory Syncytial Virus, Human genetics, Viral Proteins genetics

Abstract

Human respiratory syncytial virus (RSV) is an enveloped, nonsegmented negative-strand RNA virus of family Paramyxoviridae. RSV is the most complex member of the family in terms of the number of genes and proteins. It is also relatively divergent and distinct from the prototype members of the family. In the past 30 years, we have seen a tremendous increase in our understanding of the molecular biology of RSV based on a succession of advances involving molecular cloning, reverse genetics, and detailed studies of protein function and structure. Much remains to be learned. RSV disease is complex and variable, and the host and viral factors that determine tropism and disease are poorly understood. RSV is notable for a historic vaccine failure in the 1960s involving a formalin-inactivated vaccine that primed for enhanced disease in RSV naïve recipients. Live vaccine candidates have been shown to be free of this complication. However, development of subunit or other protein-based vaccines for pediatric use is hampered by the possibility of enhanced disease and the difficulty of reliably demonstrating its absence in preclinical studies.

Published

2013

121. Human parainfluenza virus serotypes differ in their kinetics of replication and cytokine secretion in human tracheobronchial airway epithelium.

Author

Schaap-Nutt A, Liesman R, Bartlett EJ, Scull MA, Collins PL, Pickles RJ, and Schmidt AC

Subjects

Cells, Cultured, Chemokines biosynthesis, Cytokines biosynthesis, Cytokines genetics, Host-Pathogen Interactions genetics, Host-Pathogen Interactions immunology, Humans, Interleukin-6 biosynthesis, Interleukin-6 genetics, Kinetics, Parainfluenza Virus 1, Human classification, Parainfluenza Virus 1, Human immunology, Parainfluenza Virus 1, Human pathogenicity, Parainfluenza Virus 2, Human classification, Parainfluenza Virus 2, Human immunology, Parainfluenza Virus 2, Human pathogenicity, Parainfluenza Virus 3, Human classification, Parainfluenza Virus 3, Human immunology, Parainfluenza Virus 3, Human pathogenicity, Polymorphism, Single Nucleotide, Respiratory Mucosa immunology, Respiratory Mucosa virology, Serotyping, Species Specificity, Virus Replication, Bronchi immunology, Bronchi virology, Parainfluenza Virus 1, Human physiology, Parainfluenza Virus 2, Human physiology, Parainfluenza Virus 3, Human physiology, Trachea immunology, Trachea virology

Abstract

Human parainfluenza viruses (PIVs) cause acute respiratory illness in children, the elderly, and immunocompromised patients. PIV3 is a common cause of bronchiolitis and pneumonia, whereas PIV1 and 2 are frequent causes of upper respiratory tract illness and croup. To assess how PIV1, 2, and 3 differ with regard to replication and induction of type I interferons, interleukin-6, and relevant chemokines, we infected primary human airway epithelium (HAE) cultures from the same tissue donors and examined replication kinetics and cytokine secretion. PIV1 replicated to high titer yet did not induce cytokine secretion until late in infection, while PIV2 replicated less efficiently but induced an early cytokine peak. PIV3 replicated to high titer but induced a slower rise in cytokine secretion. The T cell chemoattractants CXCL10 and CXCL11 were the most abundant chemokines induced. Differences in replication and cytokine secretion might explain some of the differences in PIV serotype-specific pathogenesis and epidemiology., (Published by Elsevier Inc.)

Published

2012

122. Molecular targets in the treatment of alcoholic hepatitis.

Author

Dhanda AD, Lee RW, Collins PL, and McCune CA

Subjects

Animals, Hepatitis, Alcoholic immunology, Humans, Tumor Necrosis Factor-alpha immunology, Hepatitis, Alcoholic drug therapy, Molecular Targeted Therapy, Pentoxifylline therapeutic use, Phosphodiesterase Inhibitors therapeutic use

Abstract

Alcohol related costs to health and society are high. One of the most serious complications of alcohol misuse to the individual is the development of alcoholic hepatitis (AH), a clinical syndrome of jaundice and progressive inflammatory liver injury in patients with a history of recent heavy alcohol use. It has a poor outcome and few existing successful therapies. The use of glucocorticoids in patients with severe AH is still controversial and there remains a group of patients with glucocorticoid-resistant disease. However, as our understanding of the pathogenesis of the condition improves there are opportunities to develop new targeted therapies with specific actions to control liver inflammation without having a detrimental effect on the immune system as a whole. In this article we review the molecular mechanisms of AH concentrating on the activation of the innate and adaptive immune response. We consider existing treatments including glucocorticoids, anti-tumor necrosis factor therapy and pentoxifylline and their limitations. Using our knowledge of the disease pathogenesis we discuss possible novel therapeutic approaches. New targets include pro-inflammatory cytokines such as interleukin (IL)-17, chemokines and their receptors (for example IL-8, CXCL9 and CXCR3) and augmentation of anti-inflammatory molecules such as IL-10 and IL-22. And there is also future potential to consider combination therapy to selectively modulate the immune response and gain control of disease.

Published

2012

123. Increased genetic and phenotypic stability of a promising live-attenuated respiratory syncytial virus vaccine candidate by reverse genetics.

Author

Luongo C, Winter CC, Collins PL, and Buchholz UJ

Subjects

Amino Acid Sequence, Animals, Base Sequence, Cell Line, Codon, DNA, Complementary metabolism, Female, Humans, Mice, Mice, Inbred BALB C, Models, Genetic, Molecular Sequence Data, Mutation, Mutation, Missense, Open Reading Frames, Pan troglodytes, Phenotype, Respiratory Syncytial Virus Infections virology, Temperature, Vaccines, Attenuated immunology, Respiratory Syncytial Virus Infections prevention & control, Respiratory Syncytial Virus Vaccines genetics, Respiratory Syncytial Viruses genetics

Abstract

Human respiratory syncytial virus (RSV) is the most important viral cause of serious pediatric respiratory illness worldwide. Currently, the most promising live-attenuated vaccine candidate is a temperature-sensitive (ts) cDNA-derived virus named rA2cp248/404/1030ΔSH, in reference to its set of attenuating mutations. In a previous clinical study, more than one-third of postvaccination nasal wash isolates exhibited partial loss of the ts phenotype. Most of this instability appeared to be due to reversion at a missense point mutation called 1030. This 1030 mutation is a single-nucleotide tyrosine-to-asparagine substitution at position 1321 (Y1321N) of the polymerase L protein that contributes to the ts and attenuation phenotypes of the vaccine candidate. The goals of the present study were to identify a reversion-resistant codon at position 1321 conferring a comparable level of attenuation and to use this to develop a genetically stable version of the vaccine virus. We modified wild-type (wt) RSV to insert each of the 20 possible amino acids at position 1321; 19 viruses were recoverable. We also investigated small deletions at or near this position, but these viruses were not recoverable. Phenotypic analysis identified alternative attenuating amino acids for position 1321. Several of these amino acids were predicted, based on the genetic code, to be refractory to deattenuation. Classical genetics, using temperature stress tests in vitro combined with nucleotide sequencing, confirmed this stability but identified a second site with a compensatory mutation at position 1313. It was possible to stabilize the 1313 site as well, providing a stable 1030 mutation. Further stress tests identified additional incidental mutations, but these did not reverse the ts/attenuation phenotype. An improved version of the vaccine candidate virus was constructed and validated in vitro by temperature stress tests and in vivo by evaluation of attenuation in seronegative chimpanzees. In addition to developing an improved version of this promising live-attenuated RSV vaccine candidate, this study demonstrated the propensity of an RNA virus to escape from attenuation but also showed that, through systematic analysis, genetics can be used to cut off the routes of escape.

Published

2012

124. Fragility fracture risk in cirrhosis: a comparison of the fracture risk assessment tool, British Society of Gastroenterology and National Institute for Health and Clinical Excellence guidelines.

Author

Ayres LRO, Clarke S, Digby-Bell J, Dhanda AD, Dharmasiri S, Caddick K, and Collins PL

Abstract

Objective: Low bone mineral density (BMD) is common in chronic liver disease and predisposes to fracture. We aimed to compare British Society of Gastroenterology (BSG) and National Institute for Health and Clinical Excellence (NICE) osteoporosis guidelines with the fracture risk assessment tool (FRAX). FRAX is a web-based algorithm used to estimate fracture risk with or without dual-emission x-ray absorptiometry (DXA). Pre-BMD FRAX categorises patients to low, intermediate or high risk according to thresholds set by the National Osteoporosis Guidelines Group (NOGG) and recommends lifestyle advice, DXA or anti-osteoporosis treatment, respectively., Design: The guidelines were applied to 132 patients with cirrhosis (91% Child-Pugh A). The number that would require DXA and be recommended treatment was determined. Using post-BMD FRAX/NOGG as a reference point, high-risk patients not recommended treatment and low-risk patients treated 'unnecessarily' were identified., Results: BSG guidelines were applicable to 100% of the cohort, 88% required DXA and 30% would be recommended treatment. Equivalent figures for NICE guidelines were 30%, 17% and 12%, and for FRAX/NOGG guidelines were 78%, 27% and 15%, respectively. Using BSG guidance 8% of high-risk patients were not recommended treatment and 62% of those treated were low risk, compared with NICE: 3%, 60% and FRAX/NOGG: 13%, 40%, respectively., Conclusion: For patients with Child-Pugh A cirrhosis BSG guidelines are the most inclusive, but have high cost implications in terms of DXA scanning and unnecessary treatment. Risk stratification using FRAX requires fewer DXA scans with minimal impact in terms of missing high-risk patients, and yields a modest reduction in unnecessary treatment.

Published

2012

125. The secreted G protein of human respiratory syncytial virus antagonizes antibody-mediated restriction of replication involving macrophages and complement.

Author

Bukreyev A, Yang L, and Collins PL

Subjects

Animals, Antibodies chemistry, Antigens chemistry, Codon, Complement System Proteins chemistry, Glycoproteins chemistry, Humans, Leukocytes cytology, Lung cytology, Macrophages cytology, Mice, Mice, Inbred BALB C, Neutralization Tests, Neutrophils cytology, Respiratory Syncytial Virus Infections metabolism, Respiratory Syncytial Virus Infections virology, Respiratory Syncytial Virus, Human immunology, Viral Envelope Proteins metabolism

Abstract

The respiratory syncytial virus (RSV) G and F glycoproteins are the neutralization antigens, and G also is expressed in a soluble form (sG). Previously, sG was demonstrated to reduce the efficiency of RSV antibody-mediated neutralization by serving as an antigen decoy and to inhibit the antibody-mediated antiviral effects of Fc receptor-bearing leukocytes. The present study demonstrated that effective antibody-mediated restriction in vivo, and the evasion of this restriction by sG, involves pulmonary macrophages and complement, but not neutrophils.

Published

2012

126. Complete genome sequence of a novel Newcastle disease virus strain isolated from a chicken in West Africa.

Author

Kim SH, Nayak S, Paldurai A, Nayak B, Samuel A, Aplogan GL, Awoume KA, Webby RJ, Ducatez MF, Collins PL, and Samal SK

Subjects

Animals, Base Sequence, Genetic Variation, Molecular Sequence Data, Newcastle disease virus classification, Newcastle disease virus isolation & purification, Sequence Analysis, DNA, Togo, Chickens virology, Genome, Viral, Newcastle Disease virology, Newcastle disease virus genetics

Abstract

The complete genome sequence of an African Newcastle disease virus (NDV) strain isolated from a chicken in Togo in 2009 was determined. The genome is 15,198 nucleotides (nt) in length and is classified in genotype VII in the class II cluster. Compared to common vaccine strains, the African strain contains a previously described 6-nt insert in the downstream untranslated region of the N gene and a novel 6-nt insert in the HN-L intergenic region. Genome length differences are a marker of the natural history of NDV. This is the first description of a class II NDV strain with a genome of 15,198 nt and a 6-nt insert in the HN-L intergenic region. Sequence divergence relative to vaccine strains was substantial, likely contributes to outbreaks, and illustrates the continued evolution of new NDV strains in West Africa.

Published

2012

127. Lineage-specific adjacent IFNG and IL26 genes share a common distal enhancer element.

Author

Collins PL, Henderson MA, and Aune TM

Subjects

Animals, Cell Lineage genetics, Cell Lineage immunology, Chromosomes, Artificial, Bacterial genetics, Conserved Sequence, Gene Order, Histones metabolism, Humans, Mice, Mice, Transgenic, Models, Genetic, Promoter Regions, Genetic, RNA Polymerase II metabolism, RNA, Untranslated genetics, RNA, Untranslated metabolism, Sequence Deletion, Th1 Cells immunology, Th17 Cells immunology, Interleukin-22, Enhancer Elements, Genetic, Evolution, Molecular, Interferon-gamma genetics, Interleukins genetics

Abstract

Certain groups of physically linked genes remain linked over long periods of evolutionary time. The general view is that such evolutionary conservation confers 'fitness' to the species. Why gene order confers 'fitness' to the species is incompletely understood. For example, linkage of IL26 and IFNG is preserved over evolutionary time yet Th17 lineages express IL26 and Th1 lineages express IFNG. We considered the hypothesis that distal enhancer elements may be shared between adjacent genes, which would require linkage be maintained in evolution. We test this hypothesis using a bacterial artificial chromosome transgenic model with deletions of specific conserved non-coding sequences. We identify one enhancer element uniquely required for IL26 expression but not for IFNG expression. We identify a second enhancer element positioned between IL26 and IFNG required for both IL26 and IFNG expression. One function of this enhancer is to facilitate recruitment of RNA polymerase II to promoters of both genes. Thus, sharing of distal enhancers between adjacent genes may contribute to evolutionary preservation of gene order.

Published

2012

128. Cutting edge: influence of Tmevpg1, a long intergenic noncoding RNA, on the expression of Ifng by Th1 cells.

Author

Collier SP, Collins PL, Williams CL, Boothby MR, and Aune TM

Subjects

Animals, Cell Differentiation genetics, Cell Differentiation immunology, Cells, Cultured, Humans, Interferon-gamma biosynthesis, Mice, Mice, Inbred BALB C, Mice, Knockout, Mice, Transgenic, RNA, Viral genetics, RNA, Viral immunology, Th1 Cells metabolism, Up-Regulation genetics, Up-Regulation immunology, Gene Expression Regulation, Viral immunology, Interferon-gamma genetics, RNA, Untranslated immunology, Th1 Cells immunology, Th1 Cells virology, Theilovirus genetics, Theilovirus immunology

Abstract

The majority of the genome is noncoding and was thought to be nonfunctional. However, it is now appreciated that transcriptional control of protein coding genes resides within these noncoding regions. Thousands of genes encoding long intergenic noncoding RNAs (lincRNAs) have been recently identified throughout the genome, which positively or negatively regulate transcription of neighboring target genes. Both TMEVPG1 and its mouse ortholog encode lincRNAs and are positioned near the IFN-γ gene (IFNG). In this study, we show that transcription of both mouse and human TMEVPG1 genes is Th1 selective and dependent on Stat4 and T-bet, transcription factors that drive the Th1 differentiation program. Ifng expression is partially restored in Stat4-/-Tbx21-/- cells through coexpression of T-bet and Tmevpg1, and Tmevpg1 expression contributes to, but alone is not sufficient to, drive Th1-dependent Ifng expression. Our results suggest that TMEVPG1 belongs to the general class of lincRNAs that positively regulate gene transcription.

Published

2012

129. Evaluation of two chimeric bovine-human parainfluenza virus type 3 vaccines in infants and young children.

Author

Karron RA, Thumar B, Schappell E, Surman S, Murphy BR, Collins PL, and Schmidt AC

Subjects

Administration, Intranasal, Adult, Antibodies, Viral blood, Child, Preschool, Hemagglutination Inhibition Tests, Humans, Infant, Parainfluenza Vaccines adverse effects, Parainfluenza Vaccines genetics, Parainfluenza Virus 3, Human genetics, Vaccination adverse effects, Vaccines, Attenuated administration & dosage, Vaccines, Attenuated adverse effects, Vaccines, Attenuated genetics, Vaccines, Attenuated immunology, Vaccines, Synthetic administration & dosage, Vaccines, Synthetic adverse effects, Vaccines, Synthetic genetics, Vaccines, Synthetic immunology, Virus Replication, Virus Shedding, Parainfluenza Vaccines administration & dosage, Parainfluenza Vaccines immunology, Parainfluenza Virus 3, Human immunology, Vaccination methods

Abstract

Human parainfluenza virus type 3 (HPIV3) is an important cause of lower respiratory tract illness in children, yet a licensed vaccine or antiviral drug is not available. We evaluated the safety, tolerability, infectivity, and immunogenicity of two intranasal, live-attenuated HPIV3 vaccines, designated rHPIV3-N(B) and rB/HPIV3, that were cDNA-derived chimeras of HPIV3 and bovine PIV3 (BPIV3). These were evaluated in adults, HPIV3 seropositive children, and HPIV3 seronegative children. A total of 112 subjects participated in these studies. Both rB/HPIV3 and rHPIV3-N(B) were highly restricted in replication in adults and seropositive children but readily infected seronegative children, who shed mean peak virus titers of 10(2.8) vs. 10(3.7)pfu/mL, respectively. Although rB/HPIV3 was more restricted in replication in seronegative children than rHPIV3-N(B), it induced significantly higher titers of hemagglutination inhibition (HAI) antibodies against HPIV3. Taken together, these data suggest that the rB/HPIV3 vaccine is the preferred candidate for further clinical development., (Copyright © 2012. Published by Elsevier Ltd.)

Published

2012

130. Pathogenesis of acute respiratory illness caused by human parainfluenza viruses.

Author

Schomacker H, Schaap-Nutt A, Collins PL, and Schmidt AC

Subjects

Bronchiolitis, Viral immunology, Bronchiolitis, Viral virology, Child, Preschool, Croup immunology, Croup virology, Humans, Immune Evasion, Immunocompromised Host, Infant, Paramyxoviridae Infections immunology, Pneumonia, Viral immunology, Pneumonia, Viral virology, Respiratory Mucosa immunology, Respiratory Mucosa pathology, Respiratory Mucosa virology, Respirovirus immunology, Bronchiolitis, Viral pathology, Croup pathology, Paramyxoviridae Infections pathology, Paramyxoviridae Infections virology, Pneumonia, Viral pathology, Respirovirus pathogenicity

Abstract

Human parainfluenza viruses (HPIVs) are a common cause of acute respiratory illness throughout life. Infants, children, and the immunocompromised are the most likely to develop severe disease. HPIV1 and HPIV2 are best known to cause croup while HPIV3 is a common cause of bronchiolitis and pneumonia. HPIVs replicate productively in respiratory epithelial cells and do not spread systemically unless the host is severely immunocompromised. Molecular studies have delineated how HPIVs evade and block cellular innate immune responses to permit efficient replication, local spread, and host-to-host transmission. Studies using ex vivo human airway epithelium have focused on virus tropism, cellular pathology and the epithelial inflammatory response, elucidating how events early in infection shape the adaptive immune response and disease outcome., (Published by Elsevier B.V.)

Published

2012

131. The human respiratory syncytial virus nonstructural protein 1 regulates type I and type II interferon pathways.

Author

Hastie ML, Headlam MJ, Patel NB, Bukreyev AA, Buchholz UJ, Dave KA, Norris EL, Wright CL, Spann KM, Collins PL, and Gorman JJ

Subjects

Animals, Catalase genetics, Catalase metabolism, Cell Line, Tumor, Chlorocebus aethiops, Cluster Analysis, Gene Expression Regulation, Host-Pathogen Interactions, Humans, Interferon Type I genetics, Interferon Type I physiology, Interferon-gamma genetics, Interferon-gamma physiology, Intracellular Signaling Peptides and Proteins genetics, Intracellular Signaling Peptides and Proteins metabolism, Oxidative Stress, Proteome genetics, Proteome metabolism, STAT1 Transcription Factor metabolism, STAT2 Transcription Factor metabolism, Signal Transduction, Superoxide Dismutase genetics, Superoxide Dismutase metabolism, Transcription, Genetic, Two-Dimensional Difference Gel Electrophoresis, Vero Cells, Interferon Type I metabolism, Interferon-gamma metabolism, Respiratory Syncytial Virus, Human physiology, Viral Nonstructural Proteins physiology

Abstract

Respiratory syncytial viruses encode a nonstructural protein (NS1) that interferes with type I and III interferon and other antiviral responses. Proteomic studies were conducted on human A549 type II alveolar epithelial cells and type I interferon-deficient Vero cells (African green monkey kidney cells) infected with wild-type and NS1-deficient clones of human respiratory syncytial virus to identify other potential pathway and molecular targets of NS1 interference. These analyses included two-dimensional differential gel electrophoresis and quantitative Western blotting. Surprisingly, NS1 was found to suppress the induction of manganese superoxide dismutase (SOD2) expression in A549 cells and to a much lesser degree Vero cells in response to infection. Because SOD2 is not directly inducible by type I interferons, it served as a marker to probe the impact of NS1 on signaling of other cytokines known to induce SOD2 expression and/or indirect effects of type I interferon signaling. Deductive analysis of results obtained from cell infection and cytokine stimulation studies indicated that interferon-γ signaling was a potential target of NS1, possibly as a result of modulation of STAT1 levels. However, this was not sufficient to explain the magnitude of the impact of NS1 on SOD2 induction in A549 cells. Vero cell infection experiments indicated that NS1 targeted a component of the type I interferon response that does not directly induce SOD2 expression but is required to induce another initiator of SOD2 expression. STAT2 was ruled out as a target of NS1 interference using quantitative Western blot analysis of infected A549 cells, but data were obtained to indicate that STAT1 was one of a number of potential targets of NS1. A label-free mass spectrometry-based quantitative approach is proposed as a means of more definitive identification of NS1 targets.

Published

2012

132. Evaluation of pneumonia virus of mice as a possible human pathogen.

Author

Brock LG, Karron RA, Krempl CD, Collins PL, and Buchholz UJ

Subjects

Adult, Animals, Antibodies, Viral immunology, Cell Line, Child, Preschool, Chlorocebus aethiops, Cross Protection, Female, Humans, Infant, Macaca mulatta, Male, Mice, Murine pneumonia virus immunology, Murine pneumonia virus pathogenicity, Pneumovirus Infections immunology, Respiratory Syncytial Viruses genetics, Respiratory Syncytial Viruses immunology, Respiratory Syncytial Viruses physiology, Young Adult, Murine pneumonia virus physiology, Pneumovirus Infections virology, Virus Replication

Abstract

Pneumonia virus of mice (PVM), a relative of human respiratory syncytial virus (RSV), causes respiratory disease in mice. There is serologic evidence suggesting widespread exposure of humans to PVM. To investigate replication in primates, African green monkeys (AGM) and rhesus macaques (n = 4) were inoculated with PVM by the respiratory route. Virus was shed intermittently at low levels by a subset of animals, suggesting poor permissiveness. PVM efficiently replicated in cultured human cells and inhibited the type I interferon (IFN) response in these cells. This suggests that poor replication in nonhuman primates was not due to a general nonpermissiveness of primate cells or poor control of the IFN response. Seroprevalence in humans was examined by screening sera from 30 adults and 17 young children for PVM-neutralizing activity. Sera from a single child (6%) and 40% of adults had low neutralizing activity against PVM, which could be consistent with increasing incidence of exposure following early childhood. There was no cross-reaction of human or AGM sera between RSV and PVM and no cross-protection in the mouse model. In native Western blots, human sera reacted with RSV but not PVM proteins under conditions in which AGM immune sera reacted strongly. Serum reactivity was further evaluated by flow cytometry using unfixed Vero cells infected with PVM or RSV expressing green fluorescent protein (GFP) as a measure of viral gene expression. The reactivity of human sera against RSV-infected cells correlated with GFP expression, whereas reactivity against PVM-infected cells was low and uncorrelated with GFP expression. Thus, PVM specificity was not evident. Our results indicate that the PVM-neutralizing activity of human sera is not due to RSV- or PVM-specific antibodies but may be due to low-affinity, polyreactive natural antibodies of the IgG subclass. The absence of PVM-specific antibodies and restriction in nonhuman primates makes PVM unlikely to be a human pathogen.

Published

2012

133. Complete genome sequences of Newcastle disease virus strains circulating in chicken populations of Indonesia.

Author

Xiao S, Paldurai A, Nayak B, Samuel A, Bharoto EE, Prajitno TY, Collins PL, and Samal SK

Subjects

Animals, Base Sequence, Molecular Sequence Data, Newcastle disease virus classification, Newcastle disease virus isolation & purification, Chickens, Genome, Viral, Newcastle Disease virology, Newcastle disease virus genetics, Poultry Diseases virology

Abstract

Eight highly virulent Newcastle disease virus (NDV) strains were isolated from vaccinated commercial chickens in Indonesia during outbreaks in 2009 and 2010. The complete genome sequences of two NDV strains and the sequences of the surface protein genes (F and HN) of six other strains were determined. Phylogenetic analysis classified them into two new subgroups of genotype VII in the class II cluster that were genetically distinct from vaccine strains. This is the first report of complete genome sequences of NDV strains isolated from chickens in Indonesia.

Published

2012

134. Mutation of the f-protein cleavage site of avian paramyxovirus type 7 results in furin cleavage, fusion promotion, and increased replication in vitro but not increased replication, tissue tropism, or virulence in chickens.

Author

Xiao S, Khattar SK, Subbiah M, Collins PL, and Samal SK

Subjects

Amino Acid Motifs, Amino Acid Sequence, Animals, Base Sequence, Cell Line, Chickens, Molecular Sequence Data, Mutation, Organ Specificity, Paramyxoviridae genetics, Paramyxoviridae Infections enzymology, Paramyxoviridae Infections virology, Poultry Diseases enzymology, Protein Processing, Post-Translational, Viral Fusion Proteins chemistry, Virulence, Furin metabolism, Paramyxoviridae pathogenicity, Paramyxoviridae physiology, Paramyxoviridae Infections veterinary, Poultry Diseases virology, Viral Fusion Proteins genetics, Viral Fusion Proteins metabolism, Virus Replication

Abstract

We constructed a reverse genetics system for avian paramyxovirus serotype 7 (APMV-7) to investigate the role of the fusion F glycoprotein in tissue tropism and virulence. The AMPV-7 F protein has a single basic residue arginine (R) at position -1 in the F cleavage site sequence and also is unusual in having alanine at position +2 (LPSSR↓FA) (underlining indicates the basic amino acids at the F protein cleavage site, and the arrow indicates the site of cleavage.). APMV-7 does not form syncytia or plaques in cell culture, but its replication in vitro does not depend on, and is not increased by, added protease. Two mutants were successfully recovered in which the cleavage site was modified to mimic sites that are found in virulent Newcastle disease virus isolates and to contain 4 or 5 basic residues as well as isoleucine in the +2 position: (RRQKR↓FI) or (RRKKR↓FI), named Fcs-4B or Fcs-5B, respectively. In cell culture, one of the mutants, Fcs-5B, formed protease-independent syncytia and grew to 10-fold-higher titers compared to the parent and Fcs-4B viruses. This indicated the importance of the single additional basic residue (K) at position -3. Syncytium formation and virus yield of the Fcs-5B virus was impaired by the furin inhibitor decanoyl-RVKR-CMK, whereas parental APMV-7 was not affected. APMV-7 is avirulent in chickens and is limited in tropism to the upper respiratory tract of 1-day-old and 2-week-old chickens, and these characteristics were unchanged for the two mutant viruses. Thus, the acquisition of furin cleavability by APMV-7 resulted in syncytium formation and increased virus yield in vitro but did not alter virus yield, tropism, or virulence in chickens.

Published

2012

135. Avian paramyxovirus serotypes 2-9 (APMV-2-9) vary in the ability to induce protective immunity in chickens against challenge with virulent Newcastle disease virus (APMV-1).

Author

Nayak B, Dias FM, Kumar S, Paldurai A, Collins PL, and Samal SK

Subjects

Administration, Intranasal, Administration, Ophthalmic, Animals, Antibodies, Neutralizing blood, Antibodies, Viral blood, Avulavirus classification, Brain virology, Chickens, Cross Reactions, Disease Models, Animal, Gastrointestinal Tract virology, Newcastle Disease mortality, Newcastle Disease virology, Respiratory System virology, Serotyping, Spleen virology, Survival Analysis, Viral Vaccines administration & dosage, Viral Vaccines immunology, Virus Shedding, Avulavirus immunology, Cross Protection, Newcastle Disease immunology, Newcastle Disease prevention & control

Abstract

The avian paramyxoviruses (APMVs) belong to the genus Avulavirus of family Paramyxoviridae. The APMVs are classified into nine serotypes on the basis of hemagglutination inhibition (HI) and neuraminidase inhibition (NI) assays, although some serologic cross-reaction exists. Newcastle disease virus (NDV), which constitutes serotype 1 (APMV-1), is an important pathogen of poultry, but the pathogenic potential of the other APMV serotypes is poorly understood. Although antibodies to APMV -2 to -9 are prevalent in chickens, the effect of prior exposure to these serotypes on susceptibility to NDV infection and disease was not known. In the present study, chickens were immunized with APMV-2 to -9 by the oculo-nasal route and later were challenged by the same route with a highly virulent strain of NDV. Among APMV-2 to -9, only APMV-3 induced serum antibodies that cross-reacted significantly with NDV and had significant NDV-neutralizing activity in vitro. In mock-immunized chickens, challenge NDV replicated throughout the respiratory tract as well as in the brain, spleen, and enteric tract. In contrast, in APMV-3-immunized chickens, challenge NDV replication was restricted to the upper respiratory tract and trachea. Some of the other APMVs also induced partial restriction of challenge NDV replication: for example, challenge NDV was not detected in the brains of APMV-9-immunized chickens, and shedding from the respiratory tract was reduced in chickens immunized with APMV-8 and -9. All of the chickens immunized with APMV-3 survived the NDV challenge; with APMV-2, -7, -8, and -9 the percentage survival was 30%, 20%, 20%, and 52.5%, respectively; whereas none of the chickens immunized with APMV-4, -5, or -6 survived. These results show that prior infection of chickens with APMV-3 induced substantial protection against NDV challenge, whereas prior infection with APMV-2, -7, -8, and -9 can alter subsequent NDV infection. The induction of NDV-neutralizing antibodies was a marker for efficient protection, but partial protection also was observed in their absence., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

136. Coordinate deletion of N-glycans from the heptad repeats of the fusion F protein of Newcastle disease virus yields a hyperfusogenic virus with increased replication, virulence, and immunogenicity.

Author

Samal S, Khattar SK, Kumar S, Collins PL, and Samal SK

Subjects

Animals, Antibodies, Viral immunology, Chickens, Glycosylation, Newcastle Disease immunology, Newcastle disease virus genetics, Newcastle disease virus immunology, Poultry Diseases immunology, Repetitive Sequences, Nucleic Acid, Viral Fusion Proteins genetics, Virulence, Virus Replication, Newcastle Disease virology, Newcastle disease virus pathogenicity, Newcastle disease virus physiology, Poultry Diseases virology, Sequence Deletion, Viral Fusion Proteins chemistry, Viral Fusion Proteins immunology

Abstract

The role of N-linked glycosylation of the Newcastle disease virus (NDV) fusion (F) protein in viral replication and pathogenesis was examined by eliminating potential acceptor sites using a reverse genetics system for the moderately pathogenic strain Beaudette C (BC). The NDV-BC F protein contains six potential acceptor sites for N-linked glycosylation at residues 85, 191, 366, 447, 471, and 541 (sites Ng1 to Ng6, respectively). The sites at Ng2 and Ng5 are present in heptad repeat (HR) domains HR1 and HR2, respectively, and thus might affect fusion. Each N-glycosylation site was eliminated individually by replacing asparagine (N) with glutamine (Q), and a double mutant (Ng2 + 5) involving the two HR domains was also made. Each mutant was successfully recovered by reverse genetics except for the one involving Ng6, which is present in the cytoplasmic domain. All of the F proteins expressed by the recovered mutant viruses were efficiently cleaved and transported to the infected-cell surface. None of the individual mutations affected viral fusogenicity, but the double mutation at Ng2 and Ng5 in HR1 and HR2 increased fusogenicity >12-fold. The single mutations at sites Ng1, Ng2, and Ng5 resulted in modestly reduced multicycle growth in vitro. These three single mutations were also the most attenuating in eggs and 1-day-old chicks and were associated with decreased replication and spread in 2-week-old chickens. In contrast, the combination of the mutations at Ng2 and Ng5 yielded a virus that, compared to the BC parent, replicated >100-fold more efficiently in vitro, was more virulent in eggs and chicks, replicated more efficiently in chickens with enhanced tropism for the brain and gut, and elicited stronger humoral cell responses. These results illustrate the effects of N-glycosylation of the F protein on NDV pathobiology and suggest that the N-glycans in HR1 and HR2 coordinately downregulate viral fusion and virulence.

Published

2012

137. Diverse functions of distal regulatory elements at the IFNG locus.

Author

Collins PL, Henderson MA, and Aune TM

Subjects

Animals, Cell Differentiation genetics, Cells, Cultured, Chromosomes, Artificial, Bacterial, Conserved Sequence, Gene Expression Regulation, Humans, Interferon-gamma biosynthesis, Mice, Mice, Inbred C57BL, Mice, Transgenic, Natural Killer T-Cells cytology, Natural Killer T-Cells immunology, Natural Killer T-Cells metabolism, Promoter Regions, Genetic, Th1 Cells cytology, Th1 Cells immunology, Th2 Cells cytology, Th2 Cells immunology, Th2 Cells metabolism, Interferon-gamma genetics, RNA, Untranslated genetics, Regulatory Sequences, Nucleic Acid, Th1 Cells metabolism

Abstract

Previous studies have identified multiple conserved noncoding sequences (CNS) at the mouse Ifng locus sufficient for enhancer activity in cell-based assays. These studies do not directly address biology of the human IFNG locus in a genomic setting. IFNG enhancers may be functionally redundant or each may be functionally unique. We test the hypothesis that each IFNG enhancer has a unique necessary function using a bacterial artificial chromosome transgenic model. We find that CNS-30, CNS-4, and CNS+20 are required at distinct stages of Th1 differentiation, whereas CNS-16 has a repressive role in Th1 and Th2 cells. CNS+20 is required for IFN-γ expression by memory Th1 cells and NKT cells. CNS-4 is required for IFN-γ expression by effector Th1 cells. In contrast, CNS-16, CNS-4, and CNS+20 are each partially required for human IFN-γ expression by NK cells. Thus, IFNG CNS enhancers have redundant necessary functions in NK cells but unique necessary functions in Th cells. These results also demonstrate that distinct CNSs are required to transcribe IFNG at each stage of the Th1 differentiation pathway.

Published

2012

138. Cholesterol-rich microdomains as docking platforms for respiratory syncytial virus in normal human bronchial epithelial cells.

Author

San-Juan-Vergara H, Sampayo-Escobar V, Reyes N, Cha B, Pacheco-Lugo L, Wong T, Peeples ME, Collins PL, Castaño ME, and Mohapatra SS

Subjects

Bronchi cytology, Cell Line, Epithelial Cells metabolism, Flow Cytometry, Fluorescent Dyes, Humans, Bronchi metabolism, Cholesterol metabolism, Membrane Fusion, Respiratory Syncytial Viruses physiology

Abstract

Respiratory syncytial virus (RSV) is one of the major causes of respiratory infections in children, and it is the main pathogen causing bronchiolitis in infants. The binding and entry mechanism by which RSV infects respiratory epithelial cells has not yet been determined. In this study, the earliest stages of RSV infection in normal human bronchial epithelial cells were probed by tracking virions with fluorescent lipophilic dyes in their membranes. Virions colocalized with cholesterol-containing plasma membrane microdomains, identified by their ability to bind cholera toxin subunit B. Consistent with an important role for cholesterol in RSV infection, cholesterol depletion profoundly inhibited RSV infection, while cholesterol repletion reversed this inhibition. Merger of the outer leaflets of the viral envelope and the cell membrane appeared to be triggered at these sites. Using small-molecule inhibitors, RSV infection was found to be sensitive to Pak1 inhibition, suggesting the requirement of a subsequent step of cytoskeletal reorganization that could involve plasma membrane rearrangements or endocytosis. It appears that RSV entry depends on its ability to dock to cholesterol-rich microdomains (lipid rafts) in the plasma membrane where hemifusion events begin, assisted by a Pak1-dependent process.

Published

2012

139. The C proteins of human parainfluenza virus type 1 block IFN signaling by binding and retaining Stat1 in perinuclear aggregates at the late endosome.

Author

Schomacker H, Hebner RM, Boonyaratanakornkit J, Surman S, Amaro-Carambot E, Collins PL, and Schmidt AC

Subjects

Animals, Blotting, Western, Chlorocebus aethiops, Humans, Immunoprecipitation, Phosphorylation, Protein Transport, STAT1 Transcription Factor antagonists & inhibitors, STAT2 Transcription Factor antagonists & inhibitors, Signal Transduction, Vero Cells, Virus Replication, Cell Nucleus metabolism, Endosomes metabolism, Interferons metabolism, STAT1 Transcription Factor metabolism, STAT2 Transcription Factor metabolism, Viral Proteins metabolism

Abstract

Interferons (IFNs) play a crucial role in the antiviral immune response. Whereas the C proteins of wild-type human parainfluenza virus type 1 (WT HPIV1) inhibit both IFN-β induction and signaling, a HPIV1 mutant encoding a single amino acid substitution (F170S) in the C proteins is unable to block either host response. Here, signaling downstream of the type 1 IFN receptor was examined in Vero cells to define at what stage WT HPIV1 can block, and F170S HPIV1 fails to block, IFN signaling. WT HPIV1 inhibited phosphorylation of both Stat1 and Stat2, and this inhibition was only slightly reduced for F170S HPIV1. Degradation of Stat1 or Stat2 was not observed. The HPIV1 C proteins were found to accumulate in the perinuclear space, often forming large granules, and co-localized with Stat1 and the cation-independent mannose 6-phosphate receptor (M6PR) that is a marker for late endosomes. Upon stimulation with IFN-β, both the WT and F170S C proteins remained in the perinuclear space, but only the WT C proteins prevented Stat1 translocation to the nucleus. In addition, WT HPIV1 C proteins, but not F170S C proteins, co-immunoprecipitated both phosphorylated and unphosphorylated Stat1. Our findings suggest that the WT HPIV1 C proteins form a stable complex with Stat1 in perinuclear granules that co-localize with M6PR, and that this direct interaction between the WT HPIV1 C proteins and Stat1 is the basis for the ability of HPIV1 to inhibit IFN signaling. The F170S mutation in HPIV1 C did not prevent perinuclear co-localization with Stat1, but apparently weakened this interaction such that, upon IFN stimulation, Stat1 was translocated to the nucleus to induce an antiviral response.

Published

2012

140. Generation by reverse genetics of an effective, stable, live-attenuated newcastle disease virus vaccine based on a currently circulating, highly virulent Indonesian strain.

Author

Xiao S, Nayak B, Samuel A, Paldurai A, Kanabagattebasavarajappa M, Prajitno TY, Bharoto EE, Collins PL, and Samal SK

Subjects

Animals, Antibodies, Viral blood, Antibodies, Viral immunology, Cell Line, Chick Embryo, Chickens immunology, Chickens virology, Cross Reactions immunology, DNA, Complementary, Gene Order, Genomic Instability, Genotype, Mutation, Newcastle Disease prevention & control, Newcastle disease virus classification, Newcastle disease virus pathogenicity, Open Reading Frames, Vaccines, Attenuated immunology, Viral Fusion Proteins chemistry, Viral Fusion Proteins genetics, Viral Tropism, Virulence, Virus Replication, Virus Shedding, Newcastle disease virus genetics, Newcastle disease virus immunology, Viral Vaccines immunology

Abstract

Newcastle disease virus (NDV) can cause severe disease in chickens. Although NDV vaccines exist, there are frequent reports of outbreaks in vaccinated chickens. During 2009-2010, despite intense vaccination, NDV caused major outbreaks among commercial poultry farms in Indonesia. These outbreaks raised concern regarding the protective immunity of current vaccines against circulating virulent strains in Indonesia. In this study, we investigated whether a recombinant attenuated Indonesian NDV strain could provide better protection against prevalent Indonesian viruses. A reverse genetics system for the highly virulent NDV strain Banjarmasin/010/10 (Ban/010) isolated in Indonesia in 2010 was constructed. The Ban/010 virus is classified in genotype VII of class II NDV, which is genetically distinct from the commercial vaccine strains B1 and LaSota, which belong to genotype II, and shares only 89 and 87% amino acid identity for the protective antigens F and HN, respectively. A mutant virus, named Ban/AF, was developed in which the virulent F protein cleavage site motif "RRQKR↓F" was modified to an avirulent motif "GRQGR↓L" by three amino acid substitutions (underlined). The Ban/AF vaccine virus did not produce syncytia or plaques in cell culture, even in the presence of added protease. Pathogenicity tests showed that Ban/AF was completely avirulent. Ban/AF replicated efficiently during 10 consecutive passages in chickens and remained genetically stable. Serological analysis showed that Ban/AF induced higher neutralization and hemagglutination inhibition antibody titers against the prevalent viruses than the commercial vaccines B1 or LaSota. Both Ban/AF and commercial vaccines provided protection against clinical disease and mortality after challenge with virulent NDV strain Ban/010 (genotype VII) or GB Texas (genotype II). However, Ban/AF significantly reduced challenge virus shedding from the vaccinated birds compared to B1 vaccine. These results suggest that Ban/AF can provide better protection than commercial vaccines and is a promising vaccine candidate against NDV strains circulating in Indonesia.

Published

2012

141. Replication, neurotropism, and pathogenicity of avian paramyxovirus serotypes 1-9 in chickens and ducks.

Author

Kim SH, Xiao S, Shive H, Collins PL, and Samal SK

Subjects

Animals, Avulavirus genetics, Avulavirus Infections virology, Cell Death physiology, Cells, Cultured, Giant Cells virology, Immunohistochemistry veterinary, Neurons virology, Ovum pathology, Ovum virology, Respiratory System virology, Serotyping veterinary, Species Specificity, Time Factors, Virulence physiology, Avulavirus pathogenicity, Avulavirus physiology, Avulavirus Infections veterinary, Bird Diseases virology, Chickens, Ducks, Viral Tropism physiology, Virus Replication physiology

Abstract

Avian paramyxovirus (APMV) serotypes 1-9 have been isolated from many different avian species. APMV-1 (Newcastle disease virus) is the only well-characterized serotype, because of the high morbidity, mortality, and economic loss caused by highly virulent strains. Very little is known about the pathogenesis, replication, virulence, and tropism of the other APMV serotypes. Here, this was evaluated for prototypes strains of APMV serotypes 2-9 in cell culture and in chickens and ducks. In cell culture, only APMV-1, -3 and -5 induced syncytium formation. In chicken DF1 cells, APMV-3 replicated with an efficiency approaching that of APMV-1, while APMV-2 and -5 replicated to lower, intermediate titers and the others were much lower. Mean death time (MDT) assay in chicken eggs and intracerebral pathogenicity index (ICPI) test in 1-day-old SPF chicks demonstrated that APMV types 2-9 were avirulent. Evaluation of replication in primary neuronal cells in vitro as well as in the brains of 1-day-old chicks showed that, among types 2-9, only APMV-3 was neurotropic, although this virus was not neurovirulent. Following intranasal infection of 1-day-old and 2-week-old chickens, replication of APMV types 2-9 was mostly restricted to the respiratory tract, although APMV-3 was neuroinvasive and neurotropic (but not neurovirulent) and also was found in the spleen. Experimental intranasal infection of 3-week-old mallard ducks with the APMVs did not produce any clinical signs (even for APMV-1) and exhibited restricted viral replication of the APMVs (including APMV-1) to the upper respiratory tract regardless of their isolation source, indicating avirulence of APMV types 1-9 in mallard ducks. The link between the presence of a furin cleavage site in the F protein, syncytium formation, systemic spread, and virulence that has been well-established with APMV-1 pathotypes was not evident with the other APMV serotypes.

Published

2012

142. Comparison of differing cytopathic effects in human airway epithelium of parainfluenza virus 5 (W3A), parainfluenza virus type 3, and respiratory syncytial virus.

Author

Zhang L, Collins PL, Lamb RA, and Pickles RJ

Subjects

Animals, Cell Line, Tumor, Humans, Parainfluenza Virus 3, Human genetics, Respiratory Syncytial Viruses genetics, Rubulavirus genetics, Virus Replication, Cytopathogenic Effect, Viral, Epithelial Cells virology, Parainfluenza Virus 3, Human physiology, Paramyxoviridae Infections virology, Respiratory Syncytial Viruses physiology, Respiratory Tract Diseases virology, Rubulavirus physiology

Abstract

Parainfluenza virus 5 (PIV5) infects a wide range of animals including dogs, pigs, cats, and humans; however, its association with disease in humans remains controversial. In contrast to parainfluenza virus 3 (PIV3) or respiratory syncytial virus (RSV), PIV5 is remarkably non-cytopathic in monolayer cultures of immortalized epithelial cells. To compare the cytopathology produced by these viruses in a relevant human tissue, we infected an in vitro model of human ciliated airway epithelium and measured outcomes of cytopathology. PIV5, PIV3 and, RSV all infected ciliated cells, and PIV5 and PIV3 infection was dependent on sialic acid residues. Only PIV5-infected cells formed syncytia. PIV5 infection resulted in a more rapid loss of infected cells by shedding of infected cells into the lumen. These studies revealed striking differences in cytopathology of PIV5 versus PIV3 or RSV and indicate the extent of cytopathology determined in cell-lines does not predict events in differentiated airway cells., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

143. Progress in understanding and controlling respiratory syncytial virus: still crazy after all these years.

Author

Collins PL and Melero JA

Subjects

Aged, Aged, 80 and over, Antibodies, Neutralizing administration & dosage, Antibodies, Neutralizing immunology, Antibodies, Viral genetics, Antibodies, Viral immunology, Antigens, Viral genetics, Antigens, Viral immunology, Antiviral Agents administration & dosage, Child, Communicable Disease Control organization & administration, Cytokines immunology, Humans, Infant, RNA, Viral genetics, RNA, Viral immunology, Respiratory Syncytial Virus Infections drug therapy, Respiratory Syncytial Virus Infections immunology, Respiratory Syncytial Virus Infections virology, Respiratory Syncytial Virus, Human genetics, Vaccines, Attenuated administration & dosage, Viral Proteins chemistry, Viral Proteins genetics, Virus Replication genetics, Virus Replication immunology, Immunity, Innate, Respiratory Syncytial Virus Infections prevention & control, Respiratory Syncytial Virus Vaccines administration & dosage, Respiratory Syncytial Virus, Human immunology, Vaccination, Viral Proteins immunology

Abstract

Human respiratory syncytial virus (RSV) is a ubiquitous pathogen that infects everyone worldwide early in life and is a leading cause of severe lower respiratory tract disease in the pediatric population as well as in the elderly and in profoundly immunosuppressed individuals. RSV is an enveloped, nonsegmented negative-sense RNA virus that is classified in Family Paramyxoviridae and is one of its more complex members. Although the replicative cycle of RSV follows the general pattern of the Paramyxoviridae, it encodes additional proteins. Two of these (NS1 and NS2) inhibit the host type I and type III interferon (IFN) responses, among other functions, and another gene encodes two novel RNA synthesis factors (M2-1 and M2-2). The attachment (G) glycoprotein also exhibits unusual features, such as high sequence variability, extensive glycosylation, cytokine mimicry, and a shed form that helps the virus evade neutralizing antibodies. RSV is notable for being able to efficiently infect early in life, with the peak of hospitalization at 2-3 months of age. It also is notable for the ability to reinfect symptomatically throughout life without need for significant antigenic change, although immunity from prior infection reduces disease. It is widely thought that re-infection is due to an ability of RSV to inhibit or subvert the host immune response. Mechanisms of viral pathogenesis remain controversial. RSV is notable for a historic, tragic pediatric vaccine failure involving a formalin-inactivated virus preparation that was evaluated in the 1960s and that was poorly protective and paradoxically primed for enhanced RSV disease. RSV also is notable for the development of a successful strategy for passive immunoprophylaxis of high-risk infants using RSV-neutralizing antibodies. Vaccines and new antiviral drugs are in pre-clinical and clinical development, but controlling RSV remains a formidable challenge., (Published by Elsevier B.V.)

Published

2011

144. Newcastle disease virus expressing human immunodeficiency virus type 1 envelope glycoprotein induces strong mucosal and serum antibody responses in Guinea pigs.

Author

Khattar SK, Samal S, Devico AL, Collins PL, and Samal SK

Subjects

AIDS Vaccines genetics, Animals, Drug Carriers, Female, Genetic Vectors, Guinea Pigs, HIV Envelope Protein gp160 genetics, HIV-1 genetics, Immunization, Secondary methods, Vaccination methods, AIDS Vaccines immunology, HIV Antibodies blood, HIV Envelope Protein gp160 immunology, HIV-1 immunology, Immunity, Mucosal, Newcastle disease virus genetics

Abstract

Human immunodeficiency virus type 1 (HIV-1) is transmitted mainly through mucosal sites. Optimum strategies to elicit both systemic and mucosal immunity are critical for the development of vaccines against HIV-1. We therefore sought to evaluate the induction of systemic and mucosal immune responses by the use of Newcastle disease virus (NDV) as a vaccine vector. We generated a recombinant NDV, designated rLaSota/gp160, expressing the gp160 envelope (Env) protein of HIV-1 from an added gene. The gp160 protein expressed by rLaSota/gp160 virus was detected on an infected cell surface and was incorporated into the NDV virion. Biochemical studies showed that gp160 present in infected cells and in the virion formed a higher-order oligomer that retained recognition by conformationally sensitive monoclonal antibodies. Expression of gp160 did not increase the virulence of recombinant NDV (rNDV) strain LaSota. Guinea pigs were administered rLaSota/gp160 via the intranasal (i.n.) or intramuscular (i.m.) route in different prime-boost combinations. Systemic and mucosal antibody responses specific to the HIV-1 envelope protein were assessed in serum and vaginal washes, respectively. Two or three immunizations via the i.n. or i.m. route induced a more potent systemic and mucosal immune response than a single immunization by either route. Priming by the i.n. route was more immunogenic than by the i.m. route, and the same was true for the boosts. Furthermore, immunization with rLaSota/gp160 by any route or combination of routes induced a Th1-type response, as reflected by the induction of stronger antigen-specific IgG2a than IgG1 antibody responses. Additionally, i.n. immunization elicited a stronger neutralizing serum antibody response to laboratory-adapted HIV-1 strain MN.3. These data illustrate that it is feasible to use NDV as a vaccine vector to elicit potent humoral and mucosal responses to the HIV-1 envelope protein.

Published

2011

145. The cDNA-derived investigational human parainfluenza virus type 3 vaccine rcp45 is well tolerated, infectious, and immunogenic in infants and young children.

Author

Karron RA, Casey R, Thumar B, Surman S, Murphy BR, Collins PL, and Schmidt AC

Subjects

Administration, Intranasal, Antibodies, Viral blood, Child, Preschool, DNA, Complementary genetics, DNA, Viral genetics, Double-Blind Method, Humans, Infant, Parainfluenza Vaccines administration & dosage, Parainfluenza Vaccines genetics, Parainfluenza Virus 3, Human genetics, Placebos administration & dosage, Vaccines, Attenuated administration & dosage, Vaccines, Attenuated adverse effects, Vaccines, Attenuated genetics, Vaccines, Attenuated immunology, Virus Shedding, Parainfluenza Vaccines adverse effects, Parainfluenza Vaccines immunology, Parainfluenza Virus 3, Human immunology

Abstract

Background: Human parainfluenza virus type 3 (HPIV3) is an important yet underappreciated cause of lower respiratory tract illness in children, and a licensed vaccine is not yet available., Methods: A live-attenuated investigational HPIV3 vaccine virus designated rcp45 was derived from cDNA by using reverse genetics. rcp45 is genetically similar to the biologically derived cp45 vaccine virus and contains all of the known attenuating mutations of cp45, but has the advantage of a short, well-characterized passage history. We evaluated the tolerability, infectivity, and immunogenicity of 2 intranasal doses of rcp45 administered 4 to 10 weeks apart in a placebo-controlled, double-blind trial. A total of 45 infants and children between 6 and 36 months of age participated in this study. Tolerability and antibody responses to vaccine or placebo were assessed in all recipients. Infectivity was assessed by quantitation of vaccine virus shedding in a subset of vaccinated children., Results: rcp45 was well tolerated and highly infectious in HPIV3-seronegative children. A second dose of vaccine administered 4 to 10 weeks after the first dose was restricted in replication and did not boost serum antibody responses. The stability of 9 cp45 mutations, including the 6 major attenuating mutations, was examined and confirmed for viral isolates from 10 children., Conclusions: The level of attenuation and immunogenicity of cDNA-derived rcp45 is comparable to what was previously observed with the biologically derived cp45 vaccine, and preliminary data suggest that the attenuating mutations in this vaccine virus are genetically stable. Continued clinical development of rcp45 is warranted.

Published

2011

146. Roles of the fusion and hemagglutinin-neuraminidase proteins in replication, tropism, and pathogenicity of avian paramyxoviruses.

Author

Kim SH, Subbiah M, Samuel AS, Collins PL, and Samal SK

Subjects

Animals, Brain pathology, Brain virology, Cell Line, Chick Embryo, Chickens, Chlorocebus aethiops, HN Protein genetics, Humans, Newcastle disease virus genetics, Protein Structure, Tertiary, Recombination, Genetic, Survival Analysis, Viral Fusion Proteins genetics, Virulence Factors genetics, Virulence Factors metabolism, HN Protein metabolism, Newcastle disease virus pathogenicity, Viral Fusion Proteins metabolism, Viral Tropism, Virus Replication

Abstract

Virulent and moderately virulent strains of Newcastle disease virus (NDV), representing avian paramyxovirus serotype 1 (APMV-1), cause respiratory and neurological disease in chickens and other species of birds. In contrast, APMV-2 is avirulent in chickens. We investigated the role of the fusion (F) and hemagglutinin-neuraminidase (HN) envelope glycoproteins in these contrasting phenotypes by designing chimeric viruses in which the F and HN glycoproteins or their ectodomains were exchanged individually or together between the moderately virulent, neurotropic NDV strain Beaudette C (BC) and the avirulent APMV-2 strain Yucaipa. When we attempted to exchange the complete F and HN glycoproteins individually and together between the two viruses, the only construct that could be recovered was recombinant APMV-2 strain Yucaipa (rAPMV-2), containing the NDV F glycoprotein in place of its own. This substitution of NDV F into APMV-2 was sufficient to confer the neurotropic, neuroinvasive, and neurovirulent phenotypes, in spite of all being at reduced levels compared to what was seen for NDV-BC. When the ectodomains of F and HN were exchanged individually and together, two constructs could be recovered: NDV, containing both the F and HN ectodomains of APMV-2; and APMV-2, containing both ectodomains of NDV. This supported the idea that homologous cytoplasmic tails and matched F and HN ectodomains are important for virus replication. Analysis of these viruses for replication in vitro, syncytium formation, mean embryo death time, intracerebral pathogenicity index, and replication and tropism in 1-day-old chicks and 2-week-old chickens showed that the two contrasting phenotypes of NDV and APMV-2 could largely be transferred between the two backbones by transfer of homotypic F and HN ectodomains. Further analysis provided evidence that the homologous stalk domain of NDV HN is essential for virus replication, while the globular head domain of NDV HN could be replaced with that of APMV-2 with only a minimal attenuating effect. These results demonstrate that the F and HN ectodomains together determine the cell fusion, tropism, and virulence phenotypes of NDV and APMV-2 and that the regions of HN that are critical to replication and the species-specific phenotypes include the cytoplasmic tail and stalk domain but not the globular head domain.

Published

2011

147. Increased sensitivity to apoptosis induced by methotrexate is mediated by JNK.

Author

Spurlock CF 3rd, Aune ZT, Tossberg JT, Collins PL, Aune JP, Huston JW 3rd, Crooke PS, Olsen NJ, and Aune TM

Subjects

Adult, Antirheumatic Agents pharmacology, Apoptosis physiology, Arthritis, Rheumatoid metabolism, Biopterins analogs & derivatives, Biopterins pharmacology, Cell Line, Tumor, Humans, Methotrexate pharmacology, Middle Aged, Reactive Oxygen Species metabolism, Tumor Cells, Cultured, Antirheumatic Agents therapeutic use, Apoptosis drug effects, Arthritis, Rheumatoid drug therapy, Gene Expression drug effects, JNK Mitogen-Activated Protein Kinases metabolism, Methotrexate therapeutic use

Abstract

Objective: Low-dose methotrexate (MTX) is an effective therapy for rheumatoid arthritis (RA), yet its mechanism of action is incompletely understood. The aim of this study was to explore the induction of apoptosis by MTX., Methods: Flow cytometry was performed to assess changes in the levels of intracellular proteins, reactive oxygen species (ROS), and apoptosis. Quantitative polymerase chain reaction was performed to assess changes in the transcript levels of select target genes in response to MTX., Results: MTX did not directly induce apoptosis but rather "primed" cells for markedly increased sensitivity to apoptosis via either mitochondrial or death receptor pathways, by a JNK-dependent mechanism. Increased sensitivity to apoptosis was mediated, at least in part, by MTX-dependent production of ROS, JNK activation, and JNK-dependent induction of genes whose protein products promote apoptosis. Supplementation with tetrahydrobiopterin blocked these MTX-induced effects. Patients with RA who were receiving low-dose MTX therapy expressed elevated levels of the JNK target gene, jun., Conclusion: Our results support a model whereby MTX inhibits reduction of dihydrobiopterin to tetrahydrobiopterin, resulting in increased production of ROS, increased JNK activity, and increased sensitivity to apoptosis. The finding of increased jun levels in patients with RA receiving low-dose MTX supports the notion that this pathway is activated by MTX in vivo and may contribute to the efficacy of MTX in inflammatory disease., (Copyright © 2011 by the American College of Rheumatology.)

Published

2011

148. Progress in the development of human parainfluenza virus vaccines.

Author

Schmidt AC, Schaap-Nutt A, Bartlett EJ, Schomacker H, Boonyaratanakornkit J, Karron RA, and Collins PL

Subjects

Acute Disease, Administration, Intranasal, Aerosols, Child, Preschool, Humans, Infant, Parainfluenza Vaccines chemistry, Parainfluenza Vaccines genetics, Respirovirus genetics, Respirovirus Infections epidemiology, Respirovirus Infections immunology, Treatment Outcome, Vaccines, Attenuated administration & dosage, Drug Design, Parainfluenza Vaccines administration & dosage, Respirovirus immunology, Respirovirus Infections prevention & control

Abstract

In children under 5 years of age, human parainfluenza viruses (HPIVs) as a group are the second most common etiology of acute respiratory illness leading to hospitalization, surpassed only by respiratory syncytial virus but ahead of influenza viruses. Using reverse genetics systems for HPIV serotypes 1, 2 and 3 (HPIV1, 2 and 3), several live-attenuated HPIVs have been generated and evaluated as intranasal vaccines in adults and in children. Two vaccines against HPIV3 were found to be well tolerated, infectious and immunogenic in Phase I trials in HPIV3-seronegative infants and children and should progress to proof-of-concept trials. Vaccines against HPIV1 and HPIV2 are less advanced and have just entered pediatric trials.

Published

2011

149. A host-restricted viral vector for antigen-specific immunization against Lyme disease pathogen.

Author

Xiao S, Kumar M, Yang X, Akkoyunlu M, Collins PL, Samal SK, and Pal U

Subjects

Animals, Antibodies, Bacterial immunology, Antibody Formation, Antigens, Bacterial biosynthesis, Antigens, Bacterial genetics, Bacterial Outer Membrane Proteins biosynthesis, Bacterial Outer Membrane Proteins genetics, Bacterial Outer Membrane Proteins immunology, Bacterial Proteins biosynthesis, Bacterial Proteins genetics, Bacterial Proteins immunology, Chickens, Cricetinae, Female, Immunization, Mice, Polymerase Chain Reaction, Antigens, Bacterial immunology, Borrelia burgdorferi genetics, Borrelia burgdorferi immunology, Genetic Vectors, Lyme Disease immunology, Lyme Disease prevention & control, Newcastle disease virus genetics

Abstract

Newcastle disease virus (NDV) is an avian virus that is attenuated in primates and is a potential vaccine vector for human use. We evaluated NDV as a vector for expressing selected antigens of the Lyme disease pathogen Borrelia burgdorferi. A series of recombinant NDVs were generated that expressed intracellular or extracellular forms of two B. burgdorferi antigens: namely, the basic membrane protein A (BmpA) and the outer surface protein C (OspC). Expression of the intracellular and extracellular forms of these antigens was confirmed in cultured chicken cells. C3H or Balb/C mice that were immunized intranasally with the NDV vectors mounted vigorous serum antibody responses against the NDV vector, but failed to mount a robust response against either the intracellular or extracellular forms of BmpA or OspC. By contrast, a single immunization of hamsters with the NDV vectors via the intranasal, intramuscular, or intraperitoneal route resulted in rapid and rigorous antibody responses against the intracellular or extracellular forms of BmpA and OspC. When groups of hamsters were separately inoculated with various NDV vectors and challenged with B. burgdorferi (10(8)cells/animal), immunization with vector expressing either intracellular or extracellular BmpA was associated with a significant reduction of the pathogen load in the joints. Taken together, our studies highlighted the importance of NDV as vaccine vector that can be used for simple yet effective immunization of hosts against bacterial infections including Lyme disease., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

150. Evaluation of the Newcastle disease virus F and HN proteins in protective immunity by using a recombinant avian paramyxovirus type 3 vector in chickens.

Author

Kumar S, Nayak B, Collins PL, and Samal SK

Subjects

Animals, Antibodies, Neutralizing blood, Antibodies, Viral blood, Chickens, Genetic Vectors genetics, HN Protein administration & dosage, HN Protein genetics, Immunization, Netherlands, Newcastle Disease mortality, Newcastle Disease prevention & control, Newcastle Disease virology, Newcastle disease virus genetics, Newcastle disease virus immunology, Newcastle disease virus pathogenicity, Poultry Diseases mortality, Poultry Diseases prevention & control, Poultry Diseases virology, Viral Fusion Proteins administration & dosage, Viral Fusion Proteins genetics, Avulavirus genetics, Genetic Vectors administration & dosage, HN Protein immunology, Newcastle Disease immunology, Poultry Diseases immunology, Recombination, Genetic, Viral Fusion Proteins immunology

Abstract

Newcastle disease virus (NDV) belongs to serotype 1 of the avian paramyxoviruses (APMV-1) and causes severe disease in chickens. Current live attenuated NDV vaccines are not fully satisfactory. An alternative is to use a viral vector vaccine that infects chickens but does not cause disease. APMV serotype 3 infects a wide variety of avian species but does not cause any apparent disease in chickens. In this study, we constructed a reverse-genetics system for recovery of infectious APMV-3 strain Netherlands from cloned cDNAs. Two recombinant viruses, rAPMV3-F and rAPMV3-HN, were generated expressing the NDV fusion (F) and hemagglutinin-neuraminidase (HN) proteins, respectively, from added genes. These viruses were used to immunize 2-week-old chickens by the oculonasal route in order to evaluate the contribution of each protein to the induction of NDV-specific neutralizing antibodies and protective immunity. Each virus induced high titers of NDV-specific hemagglutination inhibition and serum neutralizing antibodies, but the response to F protein was greater. Protective immunity was evaluated by challenging the immunized birds 21 days later with virulent NDV via the oculonasal, intramuscular, or intravenous route. With oculonasal or intramuscular challenge, all three recombinant viruses (rAPMV3, rAPMV3-F, and rAPMV3-HN) were protective, while all unvaccinated birds succumbed to death. These results indicated that rAPMV3 alone can provide cross-protection against NDV challenge. However, with intravenous challenge, birds immunized with rAPMV3 were not protected, whereas birds immunized with rAPMV3-F alone or in combination with rAPMV3-HN were completely protected, and birds immunized with rAPMV3-HN alone were partially protected. These results indicate that the NDV F and HN proteins are independent neutralization and protective antigens, but the contribution by F is greater. rAMPV3 represents an avirulent vaccine vector that can be used against NDV and other poultry pathogens.

Published

2011