Your search keyword '"Mario H. Skiadopoulos"' showing total 53 results

1. Influenza Antigens NP and M2 Confer Cross Protection to BALB/c Mice against Lethal Challenge with H1N1, Pandemic H1N1 or H5N1 Influenza A Viruses

Author

Thomas E Hickey, Sonja Leyrer, Hanné Andersen, Nathan D. Grubaugh, Nutan Mytle, Jon R Inglefield, Andrea M. Harris, Michael J. Lacy, Hang Lu, Tina Guina, Jacob T. Minang, Mario H. Skiadopoulos, and Zhidong Ma

Subjects

viruses, Cross Protection, Genetic Vectors, Hemagglutinin (influenza), medicine.disease_cause, Antibodies, Viral, Microbiology, Virus, Antigenic drift, Article, Viroporin Proteins, Viral Matrix Proteins, chemistry.chemical_compound, Influenza A Virus, H1N1 Subtype, Antigen, Orthomyxoviridae Infections, Virology, vaccine, matrix protein 1, medicine, Influenza A virus, matrix protein 2, Animals, modified Vaccinia virus Ankara (MVA), hemagglutinin, influenza A, Antigens, Viral, Pandemics, nucleoprotein, Mice, Inbred BALB C, biology, Influenza A Virus, H5N1 Subtype, Vaccination, Nucleocapsid Proteins, Influenza A virus subtype H5N1, QR1-502, Nucleoprotein, Infectious Diseases, chemistry, Influenza Vaccines, biology.protein, Female, Vaccinia, conserved antigens

Abstract

Influenza hemagglutinin (HA) is considered a major protective antigen of seasonal influenza vaccine but antigenic drift of HA necessitates annual immunizations using new circulating HA versions. Low variation found within conserved non-HA influenza virus (INFV) antigens may maintain protection with less frequent immunizations. Conserved antigens of influenza A virus (INFV A) that can generate cross protection against multiple INFV strains were evaluated in BALB/c mice using modified Vaccinia virus Ankara (MVA)-vectored vaccines that expressed INFV A antigens hemagglutinin (HA), matrix protein 1 (M1), nucleoprotein (NP), matrix protein 2 (M2), repeats of the external portion of M2 (M2e) or as tandem repeats (METR), and M2e with transmembrane region and cytoplasmic loop (M2eTML). Protection by combinations of non-HA antigens was equivalent to that of subtype-matched HA. Combinations of NP and forms of M2e generated serum antibody responses and protected mice against lethal INFV A challenge using PR8, pandemic H1N1 A/Mexico/4108/2009 (pH1N1) or H5N1 A/Vietnam/1203/2004 (H5N1) viruses, as demonstrated by reduced lung viral burden and protection against weight loss. The highest levels of protection were obtained with NP and M2e antigens delivered as MVA inserts, resulting in broadly protective immunity in mice and enhancement of previous natural immunity to INFV A.

Published

2021

2. Correlation between anthrax lethal toxin neutralizing antibody levels and survival in guinea pigs and nonhuman primates vaccinated with the AV7909 anthrax vaccine candidate

Author

Daniel C. Sanford, Na Li, Vladimir Savransky, Gloria S. Sivko, Gregory V. Stark, Michael J. Lacy, Mario H. Skiadopoulos, Melicia Gainey, Boris Ionin, and Jeffry D. Shearer

Subjects

0301 basic medicine, Primates, Guinea Pigs, Anthrax Vaccines, Article, 03 medical and health sciences, Ames strain, 0302 clinical medicine, Immune system, Animals, 030212 general & internal medicine, Neutralizing antibody, Anthrax vaccines, General Veterinary, General Immunology and Microbiology, biology, Lethal dose, Vaccination, Public Health, Environmental and Occupational Health, Anthrax Vaccine Adsorbed, biology.organism_classification, Virology, Antibodies, Neutralizing, Bacillus anthracis, 030104 developmental biology, Infectious Diseases, Immunology, biology.protein, Molecular Medicine, Antibody, Post-Exposure Prophylaxis

Abstract

The anthrax vaccine candidate AV7909 is being developed as a next generation vaccine for a post-exposure prophylaxis (PEP) indication against anthrax. AV7909 consists of the Anthrax Vaccine Adsorbed (AVA, BioThrax®) bulk drug substance adjuvanted with the immunostimulatory oligodeoxynucleotide (ODN) compound, CPG 7909. The addition of CPG 7909 to AVA enhances both the magnitude and the kinetics of antibody responses in animals and human subjects, making AV7909 a suitable next-generation vaccine for use in a PEP setting. The studies described here provide initial information on AV7909-induced toxin-neutralizing antibody (TNA) levels associated with the protection of animals from lethal Bacillus anthracis challenge. Guinea pigs or nonhuman primates (NHPs) were immunized on Days 0 and 28 with various dilutions of AV7909, AVA or a saline or Alhydrogel + CPG 7909 control. Animals were challenged via the inhalational route with a lethal dose of aerosolized B. anthracis (Ames strain) spores and observed for clinical signs of disease and mortality. The relationship between pre-challenge serum TNA levels and survival following challenge was determined in order to calculate a threshold TNA level associated with protection. Immunisation with AV7909 induced a rapid, highly protective TNA response in guinea pigs and NHPs. Surprisingly, the TNA threshold associated with a 70% probability of survival for AV7909 immunized animals was substantially lower than the threshold which has been established for the licensed AVA vaccine. The results of this study suggest that the TNA threshold of protection against anthrax could be modified by the addition of an immune stimulant such as CPG 7909 and that the TNA levels associated with protection may be vaccine-specific.

Published

2017

3. Evaluation of Immunogenicity and Efficacy of Anthrax Vaccine Adsorbed for Postexposure Prophylaxis

Author

Ekaterina Vert-Wong, Suha Sari, Thomas L. Rudge, Robert J. Hopkins, Tina Guina, Frances M. Reid, Cris Howard, Gregory V. Stark, Jeffrey G. Smith, Boris Ionin, Gloria S. Sivko, Virginia Johnson, Kristin H. Clement, M. Lisa Swoboda, Gary S. Nabors, Mario H. Skiadopoulos, Brett Pleune, and Alison Innes

Subjects

Adult, Male, Microbiology (medical), Adolescent, medicine.medical_treatment, Clinical Biochemistry, Immunology, Anthrax Vaccines, Anthrax, Young Adult, Animal data, medicine, Animals, Humans, Immunology and Allergy, Post-exposure prophylaxis, Aged, Vaccines, Anthrax vaccines, biology, business.industry, Immunogenicity, fungi, Vaccination, Antibody titer, Anthrax Vaccine Adsorbed, Middle Aged, biology.organism_classification, Antibodies, Bacterial, Antibodies, Neutralizing, Survival Analysis, Virology, Bacillus anthracis, Disease Models, Animal, Macaca fascicularis, Female, Antitoxins, Rabbits, Post-Exposure Prophylaxis, business

Abstract

Antimicrobials administered postexposure can reduce the incidence or progression of anthrax disease, but they do not protect against the disease resulting from the germination of spores that may remain in the body after cessation of the antimicrobial regimen. Such additional protection may be achieved by postexposure vaccination; however, no anthrax vaccine is licensed for postexposure prophylaxis (PEP). In a rabbit PEP study, animals were subjected to lethal challenge with aerosolized Bacillus anthracis spores and then were treated with levofloxacin with or without concomitant intramuscular (i.m.) vaccination with anthrax vaccine adsorbed (AVA) (BioThrax; Emergent BioDefense Operations Lansing LLC, Lansing, MI), administered twice, 1 week apart. A significant increase in survival rates was observed among vaccinated animals compared to those treated with antibiotic alone. In preexposure prophylaxis studies in rabbits and nonhuman primates (NHPs), animals received two i.m. vaccinations 1 month apart and were challenged with aerosolized anthrax spores at day 70. Prechallenge toxin-neutralizing antibody (TNA) titers correlated with animal survival postchallenge and provided the means for deriving an antibody titer associated with a specific probability of survival in animals. In a clinical immunogenicity study, 82% of the subjects met or exceeded the prechallenge TNA value that was associated with a 70% probability of survival in rabbits and 88% probability of survival in NHPs, which was estimated based on the results of animal preexposure prophylaxis studies. The animal data provide initial information on protective antibody levels for anthrax, as well as support previous findings regarding the ability of AVA to provide added protection to B. anthracis -infected animals compared to antimicrobial treatment alone.

Published

2013

4. Recombinant human parainfluenza virus type 2 with mutations in V that permit cellular interferon signaling are not attenuated in non-human primates

Author

Konrad C. Bradley, Christopher D'Angelo, Alexander C. Schmidt, Shenelle-Marie Wise, Peter L. Collins, Olivia S. Kim, Caraline Higgins, Mario H. Skiadopoulos, Brian R. Murphy, Reina Mayor, Sheila M. Nolan, Anne Schaap-Nutt, Emerito Amaro-Carambot, and Stephanie D. Davis

Subjects

Primates, Genes, Viral, Mutant, Virus Replication, medicine.disease_cause, Article, Virus, Cell Line, Open Reading Frames, Viral Proteins, Species Specificity, Interferon, Virology, Chlorocebus aethiops, medicine, Animals, Humans, STAT2, Vero Cells, Mutation, Base Sequence, biology, Phosphoproteins, Macaca mulatta, Molecular biology, Recombinant Proteins, Parainfluenza Virus 2, Human, DNA-Binding Proteins, Viral replication, Phosphoprotein, DNA, Viral, Host-Pathogen Interactions, Interferon Type I, biology.protein, Interferons, Interferon type I, Signal Transduction, medicine.drug

Abstract

The HPIV2 V protein inhibits type I interferon (IFN) induction and signaling. To manipulate the V protein, whose coding sequence overlaps that of the polymerase-associated phosphoprotein (P), without altering the P protein, we generated an HPIV2 virus in which P and V are expressed from separate genes (rHPIV2-P+V). rHPIV2-P+V replicated like HPIV2-WT in vitro and in non-human primates. HPIV2-P+V was modified by introducing two separate mutations into the V protein to create rHPIV2-L101E/L102E and rHPIV2-Delta122-127. In contrast to HPIV2-WT, both mutant viruses were unable to degrade STAT2, leaving virus-infected cells susceptible to IFN. Neither mutant, nor HPIV2-WT, induced significant amounts of IFN-beta in infected cells. Surprisingly, neither rHPIV2-L101E/L102E nor rHPIV2-Delta122-127 was attenuated in two species of non-human primates. This indicates that loss of HPIV2's ability to inhibit IFN signaling is insufficient to attenuate virus replication in vivo as long as IFN induction is still inhibited.

Published

2010

5. A novel human parainfluenza virus type 1 (HPIV1) with separated P and C genes is useful for generating C gene mutants for evaluation as live-attenuated virus vaccine candidates

Author

Janice Esker, Peter L. Collins, Jim Boonyaratanakornkit, Ann-Marie Cruz, Mario H. Skiadopoulos, Alexander C. Schmidt, Adam Castaño, Emmalene J. Bartlett, and Brian R. Murphy

Subjects

Paramyxoviridae, Molecular Sequence Data, Mutant, Apoptosis, Gene Mutant, Gene mutation, Antibodies, Viral, Vaccines, Attenuated, Virus Replication, Article, Virus, Cell Line, Viral Proteins, Chlorocebus aethiops, Animals, Humans, Mononegavirales, Parainfluenza Vaccines, Sequence Deletion, Vaccines, Synthetic, Attenuated vaccine, Base Sequence, Virulence, General Veterinary, General Immunology and Microbiology, biology, Public Health, Environmental and Occupational Health, Wild type, Viral Load, Phosphoproteins, biology.organism_classification, Virology, Parainfluenza Virus 1, Human, Infectious Diseases, Interferon Type I, Molecular Medicine

Abstract

A novel recombinant human parainfluenza virus type 1 (rHPIV1), rHPIV1-C+P, in which the overlapping open reading frames of the C and P genes were separated in order to introduce mutations into the C gene without affecting P, was generated. Infectious rHPIV1-C+P was readily recovered and replicated as efficiently as HPIV1 wild type (wt) in vitro and in African green monkeys (AGMs). rHPIV1-C+P expressed increased levels of C protein and, surprisingly, activated the type I IFN and apoptosis responses more strongly than HPIV1 wt. rHPIV1-C+P provided a useful backbone for recovering an attenuated P/C gene mutation (Delta 84-85), which was previously unrecoverable, likely due to detrimental effects of the deletion on the P protein. rHPIV1-C(Delta 84-85)+P and an additional mutant, rHPIV1-C(Delta 169-170)+P, were found to replicate to similar titers in vitro and to activate the type I IFN and apoptosis responses to a similar degree as rHPIV1-C+P. rHPIV1-C(Delta 84-85)+P was found to be highly attenuated in AGMs, and all viruses were immunogenic and effective in protecting AGMs against challenge with HPIV1 wt. rHPIV1-C(Delta 84-85)+P will be investigated as a potential live-attenuated vaccine candidate for HPIV1.

Published

2010

6. Recombinant human parainfluenza virus type 2 vaccine candidates containing a 3′ genomic promoter mutation and L polymerase mutations are attenuated and protective in non-human primates

Author

Konrad C. Bradley, Stacia Bier, Marisa St. Claire, Stephanie D. Davis, Randy Elkins, Anne Schaap-Nutt, Mario H. Skiadopoulos, Olivia S. Kim, Brian R. Murphy, Sheila M. Nolan, Emerito Amaro-Carambot, Peter L. Collins, and Sonja R. Surman

Subjects

Respiratory System, Mutant, Biology, Vaccines, Attenuated, Virus Replication, medicine.disease_cause, Article, Virus, Cell Line, Viral Proteins, Parainfluenza virus type 2, Cricetinae, medicine, Animals, Humans, Promoter Regions, Genetic, Parainfluenza Vaccines, Polymerase, Vaccines, Synthetic, Mutation, Mesocricetus, General Veterinary, General Immunology and Microbiology, Temperature, Public Health, Environmental and Occupational Health, Macaca mulatta, Virology, Molecular biology, Reverse genetics, Parainfluenza Virus 2, Human, Human Parainfluenza Virus, Infectious Diseases, Viral replication, biology.protein, Molecular Medicine

Abstract

Previously, we identified several attenuating mutations in the L polymerase protein of human parainfluenza virus type 2 (HPIV2) and genetically stabilized those mutations using reverse genetics [Nolan SM, Surman S, Amaro-Carambot E, Collins PL, Murphy BR, Skiadopoulos MH. Live-attenuated intranasal parainfluenza virus type 2 vaccine candidates developed by reverse genetics containing L polymerase protein mutations imported from heterologous paramyxoviruses. Vaccine 2005;39(23):4765-74]. Here we describe the discovery of an attenuating mutation at nucleotide 15 (15(T-->C)) in the 3' genomic promoter that was also present in the previously characterized mutants. We evaluated the properties of this promoter mutation alone and in various combinations with the L polymerase mutations. Amino acid substitutions at L protein positions 460 (460A or 460P) or 948 (948L), or deletion of amino acids 1724 and 1725 (Delta1724), each conferred a temperature sensitivity (ts) phenotype whereas the 15(T-->C) mutation did not. The 460A and 948L mutations each contributed to restricted replication in the lower respiratory tract of African green monkeys, but the Delta1724 mutation increased attenuation only in certain combinations with other mutations. We constructed two highly attenuated viruses, rV94(15C)/460A/948L and rV94(15C)/948L/Delta1724, that were immunogenic and protective against challenge with wild-type HPIV2 in African green monkeys and, therefore, appear to be suitable for evaluation in humans.

Published

2007

7. An improved method for the recovery of recombinant paramyxovirus vaccine candidates suitable for use in human clinical trials

Author

Sonja R. Surman, Mario H. Skiadopoulos, Brian R. Murphy, and Peter L. Collins

Subjects

DNA, Complementary, Paramyxoviridae, viruses, Vaccines, Attenuated, Virus, Virology, Chlorocebus aethiops, Animals, Humans, Mononegavirales, Vero Cells, Recombination, Genetic, Clinical Trials as Topic, biology, Electroporation, fungi, Viral Vaccines, Transfection, biology.organism_classification, Reverse genetics, Parainfluenza Virus 1, Human, Parainfluenza Virus 2, Human, Parainfluenza Virus 3, Human, Kinetics, Paramyxovirus vaccine, Vero cell, Paramyxovirinae, Plasmids

Abstract

We describe a method for the generation of clinical grade, live-attenuated vaccines in Vero cells entirely from cDNA plasmids. The entire electroporation procedure can be completed in less than 15 minutes and this is a significant improvement over previous lipid or electroporation based transfection techniques that also involve a heat-shock step. Importantly, the virus preparations can be generated with a minimal use of animal product derived materials, an important consideration for a vaccine candidate that is to be tested in humans. Since it is likely that all live-attenuated parainfluenza virus and pneumovirus vaccines in the future will be generated using reverse genetics, this simplified method provides guidance on how this can be achieved.

Published

2007

8. Nonsegmented Negative-Strand Viruses as Vaccine Vectors

Author

Alexander Bukreyev, Mario H. Skiadopoulos, Peter L. Collins, and Brian R. Murphy

Subjects

biology, Paramyxoviridae, viruses, Immunology, Filoviridae, Rhabdoviridae, biology.organism_classification, Microbiology, Virology, Virus, Sendai virus, Vesicular stomatitis virus, Insect Science, Minireview, Mononegavirales, Oncovirus

Abstract

The live-virus vector era began in 1983, when Smith, Mackett, and Moss constructed a recombinant vaccinia virus expressing hepatitis B surface antigen and demonstrated the induction of hepatitis B-specific antibodies in rabbits immunized with the recombinant virus (113). Subsequently, live-virus vectors were developed with other DNA viruses, such as adenoviruses and herpesviruses, and with positive-strand RNA viruses, such as alphaviruses and flaviviruses. The vaccine vector potential of the large group of nonsegmented negative-strand RNA viruses (NNSV) remained unexplored largely due to the lack of infectivity of their genomic RNA in cell culture and the absence of a mechanism for recombinational insertion of foreign genes. The NNSV (order Mononegavirales) comprise four families: Rhabdoviridae, represented by vesicular stomatitis virus (VSV) and rabies virus (RV); Paramyxoviridae, including Sendai virus (SeV), human parainfluenza virus types 1, 2, 3, and 4 (HPIV1 to -4), measles and mumps viruses, Newcastle disease virus (NDV), and human respiratory syncytial and metapneumoviruses (HRSV and HMPV); Filoviridae, containing Ebola and Marburg viruses; and Bornaviridae, containing Borna disease virus. In 1994, Schnell, Mebatsion, and Conzelmann developed a reverse genetic system for RV that allowed the recovery of infectious virus entirely from cloned cDNA (102). This was followed quickly by the development of reverse genetic systems for numerous other NNSV (17, 22, 33, 50, 55, 69, 73, 76, 83, 133). This review will focus on the use of NNSV, in particular members of the Rhabdoviridae and Paramyxoviridae, as live vaccine vectors.

Published

2006

9. Attenuating mutations in the P/C gene of human parainfluenza virus type 1 (HPIV1) vaccine candidates abrogate the inhibition of both induction and signaling of type I interferon (IFN) by wild-type HPIV1

Author

William Van Cleve, Mario H. Skiadopoulos, Joseph Bekisz, Sonja R. Surman, Peter L. Collins, Kathryn C. Zoon, Brian R. Murphy, Emerito Amaro-Carambot, and Emmalene J. Bartlett

Subjects

Mutant, Context (language use), Biology, Vaccines, Attenuated, Human parainfluenza virus, Cell Line, Viral Proteins, Interferon, Virology, Chlorocebus aethiops, Attenuating mutation, medicine, Animals, Humans, Point Mutation, Parainfluenza Vaccines, Vero Cells, A549 cell, Wild type, Interferon antagonist, Phosphoproteins, In vitro, Parainfluenza Virus 1, Human, Interferon Type I, Vero cell, Antagonism, Signal Transduction, medicine.drug, Vaccine candidate

Abstract

Recombinant human parainfluenza virus type 1 (HPIV1) and mutants containing point and deletion (Δ) mutations in the P/C gene (r-C Δ10–15 HN T553A , r-C R84G , r-C F170S and r-C Δ170 ), which have previously been evaluated as HPIV1 vaccine candidates, were evaluated for their effect on the type I interferon (IFN) response in vitro. HPIV1 wt infection inhibited the IFN response by inhibiting IFN regulatory factor-3 (IRF-3) activation and IFN production in A549 cells and IFN signaling in Vero cells. In contrast, r-C R84G , r-C F170S and r-C Δ170 were defective for inhibition of IRF-3 activation and IFN production and r-C F170S and r-C Δ170 did not inhibit IFN signaling. Thus, HPIV1 antagonizes the IFN response at both the level of induction and signaling, and antagonism at both levels was disrupted by mutations in the P/C gene. Because C F170S affects C and not P, the anti-IFN function can be attributed to the C proteins. These data, in the context of previous in vivo studies, suggest that the loss of antagonism of the IFN response at both the level of induction and signaling, observed with the P/C mutants, r-C F170S and r-C Δ170 , was necessary for significant attenuation in African green monkeys (AGMs).

Published

2006

10. Individual contributions of the human metapneumovirus F, G, and SH surface glycoproteins to the induction of neutralizing antibodies and protective immunity

Author

Stéphane Biacchesi, Peter L. Collins, Mario H. Skiadopoulos, Sonja R. Surman, Brian R. Murphy, Ursula J. Buchholz, and Emerito Amaro-Carambot

Subjects

G protein, Protective immunity, viruses, Genetic Vectors, Molecular Sequence Data, Neutralizing antibodies, Antibodies, Viral, Neutralization, Viral Proteins, Human metapneumovirus, Antigen, Neutralization Tests, Immunity, Cricetinae, Virology, Animals, Humans, Glycoproteins, Recombination, Genetic, chemistry.chemical_classification, Membrane Glycoproteins, Paramyxoviridae Infections, Base Sequence, Mesocricetus, biology, virus diseases, biology.organism_classification, Reverse genetics, Parainfluenza Virus 1, Human, respiratory tract diseases, chemistry, biology.protein, Metapneumovirus, Glycoprotein, Antibody

Abstract

We evaluated the individual contributions of the three surface glycoproteins of human metapneumovirus (HMPV), namely the fusion F, attachment G, and small hydrophobic SH proteins, to the induction of serum HMPV-binding antibodies, serum HMPV-neutralizing antibodies, and protective immunity. Using reverse genetics, each HMPV protein was expressed individually from an added gene in recombinant human parainfluenza virus type 1 (rHPIV1) and used to infect hamsters once or twice by the intranasal route. The F protein was highly immunogenic and protective, whereas G and SH were only weakly or negligibly immunogenic and protective, respectively. Thus, in contrast to other paramyxoviruses, the HMPV attachment G protein is not a major neutralization or protective antigen. Also, although the SH protein of HMPV is a virion protein that is much larger than its counterparts in previously studied paramyxoviruses, it does not appear to be a significant neutralization or protective antigen.

Published

2006

11. Infection of Nonhuman Primates with Recombinant Human Metapneumovirus Lacking the SH, G, or M2-2 Protein Categorizes Each as a Nonessential Accessory Protein and Identifies Vaccine Candidates

Author

Peter L. Collins, Mario H. Skiadopoulos, Brian R. Murphy, Quynh N. Pham, Stéphane Biacchesi, and Ursula J. Buchholz

Subjects

Genes, Viral, viruses, Immunology, Virus Replication, Microbiology, Virus, law.invention, Viral Proteins, Human metapneumovirus, law, Virology, Chlorocebus aethiops, Animals, Antigens, Viral, Respiratory Tract Infections, Gene, Recombination, Genetic, Paramyxoviridae Infections, biology, virus diseases, Viral Vaccines, Vaccine efficacy, biology.organism_classification, Reverse genetics, respiratory tract diseases, Disease Models, Animal, Open reading frame, Viral replication, Insect Science, Recombinant DNA, Pathogenesis and Immunity, Immunization, Metapneumovirus, Gene Deletion

Abstract

Recombinant human metapneumovirus (HMPV) in which the SH, G, or M2 gene or open reading frame was deleted by reverse genetics was evaluated for replication and vaccine efficacy following topical administration to the respiratory tract of African green monkeys, a permissive primate host. Replication of the ΔSH virus was only marginally less efficient than that of wild-type HMPV, whereas the ΔG and ΔM2-2 viruses were reduced sixfold and 160-fold in the upper respiratory tract and 3,200-fold and 4,000-fold in the lower respiratory tract, respectively. Even with the highly attenuated mutants, there was unequivocal HMPV replication at each anatomical site in each animal. Thus, none of these three proteins is essential for HMPV replication in a primate host, although G and M2-2 increased the efficiency of replication. Each gene-deletion virus was highly immunogenic and protective against wild-type HMPV challenge. The ΔG and ΔM2-2 viruses are promising vaccine candidates that are based on independent mechanisms of attenuation and are appropriate for clinical evaluation.

Published

2005

12. Live-attenuated intranasal parainfluenza virus type 2 vaccine candidates developed by reverse genetics containing L polymerase protein mutations imported from heterologous paramyxoviruses

Author

Sonja R. Surman, Mario H. Skiadopoulos, Brian R. Murphy, Sheila M. Nolan, Peter L. Collins, and Emerito Amaro-Carambot

Subjects

Paramyxoviridae, Molecular Sequence Data, Heterologous, Vaccines, Attenuated, Virus Replication, medicine.disease_cause, Virus, Cell Line, Parainfluenza virus type 2, Cricetinae, medicine, Animals, Humans, Amino Acid Sequence, Codon, Mononegavirales, Parainfluenza Vaccines, Administration, Intranasal, Polymerase, Vaccines, Synthetic, Mutation, Mesocricetus, General Veterinary, General Immunology and Microbiology, biology, Public Health, Environmental and Occupational Health, DNA-Directed RNA Polymerases, biology.organism_classification, Virology, Reverse genetics, Parainfluenza Virus 2, Human, Infectious Diseases, biology.protein, Paramyxovirinae, Molecular Medicine

Abstract

Live-attenuated recombinant human parainfluenza virus type 2 (rHPIV2) vaccine candidates were created using reverse genetics by importing known attenuating mutations in the L polymerase protein from heterologous paramyxoviruses into the homologous sites of the HPIV2 L protein. Four recombinants (rF460L, rY948H, rL1566I, and rS1724I) were recovered and three were attenuated for replication in hamsters. The genetic stability of the imported mutations at three of the four sites was enhanced by use of alternative codons or by deletion of a pair of amino acids. rHPIV2s bearing these modified mutations exhibited enhanced attenuation. The genetically stabilized mutations conferring a high level of attenuation will be useful in generating a live-attenuated virus vaccine for HPIV2.

Published

2005

13. Recovery of human metapneumovirus from cDNA: optimization of growth in vitro and expression of additional genes

Author

Kim C. Tran, Peter L. Collins, Mario H. Skiadopoulos, Brian R. Murphy, Stéphane Biacchesi, and Ursula J. Buchholz

Subjects

Expression vector, DNA, Complementary, Time Factors, Sequence analysis, viruses, Green Fluorescent Proteins, Genome, Viral, Biology, Recombinant virus, Virus, Cell Line, Paramyxovirus, Human metapneumovirus, Virology, Complementary DNA, Consensus sequence, Animals, Humans, Trypsin, Promoter Regions, Genetic, Gene, Respiratory disease, Recombination, Genetic, Vaccines, biology.organism_classification, Molecular biology, Luminescent Proteins, Metapneumovirus, Reassortant Viruses

Abstract

Human metapneumovirus (HMPV) is a recently recognized causative agent of respiratory tract disease in individuals of all ages and especially young infants. HMPV remains poorly characterized and has been reported to replicate inefficiently in vitro. Complete consensus sequences were recently determined for two isolates representing the two proposed HMPV genetic subgroups (Biacchesi et al., Virology 315 (1) (2003) 1). We have developed a reverse genetic system to produce one of these isolates, CAN97-83, entirely from cDNA. We also recovered a version, rHMPV–GFP, in which the enhanced green fluorescent protein (GFP) was expressed from a transcription cassette inserted as the first gene, leaving the 41-nt leader region and first 16 nt of the N gene undisturbed. The ability to monitor GFP expression in living cells greatly facilitated the initial recovery of this slow-growing virus. In addition, the ability to express a foreign gene from an engineered transcription cassette confirmed the identification of the HMPV transcription signals and identified the F gene-end signal as being highly efficient for transcription termination. The ability to recover virus containing a foreign insert in this position indicated that the viral promoter is contained within the 3′-terminal 57 nt of the genome. Recombinant HMPV replicated in vitro as efficiently as biologically derived HMPV, whereas the kinetics and final yield of rHMPV–GFP were reduced several-fold. Conditions for trypsin treatment were investigated, providing for improved virus yields. Another version of HMPV, rHMPV+G1F23, was recovered that contained a second copy of the G gene and two extra copies of F in promoter-proximal positions in the order G1–F2–F3. Thus, this recombinant genome would encode 11 mRNAs rather than eight and would be 17.3 kb long, 30% longer than that of the natural virus. Nonetheless, the rHMPV+G1F23 virus replicated in vitro with an efficiency that was only modestly reduced compared to rHMPV and was essentially the same as rHMPV–GFP. Northern blot analysis showed that the increased number and promoter-proximal location of the added copies of the F and G genes resulted in a more than 6- and 14-fold increase in the expression of F and G mRNA, respectively, and sequence analysis confirmed the intactness of the added genes in recovered virus. Thus, it should be feasible to construct an HMPV vaccine virus containing extra copies of the G and F putative protective antigen genes to increase antigen expression or to provide representation of additional antigenic lineages or subgroups of HMPV.

Published

2004

14. Determinants of the Host Range Restriction of Replication of Bovine Parainfluenza Virus Type 3 in Rhesus Monkeys Are Polygenic

Author

Peter L. Collins, William R. Elkins, Mario H. Skiadopoulos, Alexander Schmidt, Brian R. Murphy, Jeffrey M. Riggs, Marisa St. Claire, and Sonja R. Surman

Subjects

DNA, Complementary, Immunology, Biology, Virus Replication, Microbiology, Cell Line, law.invention, Open Reading Frames, law, Virology, Vaccines and Antiviral Agents, Animals, Humans, ORFS, Gene, Pathogen, Parainfluenza Virus 3, Bovine, Chimera, Point mutation, Temperature, Macaca mulatta, Parainfluenza Virus 3, Human, Open reading frame, Viral replication, Insect Science, Recombinant DNA, biology.protein, Antibody

Abstract

The Kansas strain of bovine parainfluenza virus type 3 (BPIV3) is 100- to 1,000-fold restricted in replication in the respiratory tracts of nonhuman primates compared to human PIV3 (HPIV3), an important pathogen of infants and young children. BPIV3 is also restricted in replication in human infants and children, yet it is immunogenic and is currently being evaluated in clinical trials as a vaccine candidate to protect against illness caused by HPIV3. We have examined the genetic basis for the host range attenuation phenotype of BPIV3 by exchanging each open reading frame (ORF) of a recombinant wild-type HPIV3 with the analogous ORF from BPIV3, with the caveats that the multiple ORFs of the P gene were exchanged as a single unit and that the HN and F genes were exchanged as a single unit. Recombinant chimeric bovine-human PIV3s were recovered from cDNA, and the levels of viral replication in vitro and in the respiratory tract of rhesus monkeys were determined. Recombinant chimeric HPIV3s bearing the BPIV3 N or P ORF were highly attenuated in the upper and lower respiratory tracts of monkeys, whereas those bearing the BPIV3 M or L ORF or the F and HN genes were only moderately attenuated. This indicates that the genetic determinants of the host range restriction of replication of BPIV3 for primates are polygenic, with the major determinants being the N and P ORFs. Monkeys immunized with these bovine-human chimeric viruses, including the more highly attenuated ones, developed higher levels of HPIV3 hemagglutination-inhibiting serum antibodies than did monkeys immunized with BPIV3 and were protected from challenge with wild-type HPIV3. Furthermore, host range determinants could be combined with attenuating point mutations to achieve an increased level of attenuation. Thus, chimeric recombinant bovine-human PIV3 viruses that manifest different levels of attenuation in rhesus monkeys are available for evaluation as vaccine candidates to protect infants from the severe lower respiratory tract disease caused by HPIV3.

Published

2003

15. More antibody with less antigen: Can immunogenicity of attenuated live virus vaccines be improved?

Author

Peter L. Collins, Alexander Bukreyev, Alexander C. Schmidt, Mario H. Skiadopoulos, Brian R. Murphy, and Josephine M. McAuliffe

Subjects

T-Lymphocytes, viruses, Antibodies, Viral, Lymphocyte Activation, Vaccines, Attenuated, Virus Replication, Recombinant virus, Virus, Interferon-gamma, Animals, Vaccines, Synthetic, Multidisciplinary, Attenuated vaccine, biology, Viral culture, Viral Vaccine, Immunogenicity, Granulocyte-Macrophage Colony-Stimulating Factor, Viral Vaccines, RNA virus, Biological Sciences, biology.organism_classification, Macaca mulatta, Virology, Parainfluenza Virus 3, Human, Viral replication, Immunology

Abstract

New or improved vaccines against viruses such as influenza, parainfluenza types 1–3, measles, dengue, and respiratory syncytial virus would prevent an enormous burden of morbidity and mortality. Vaccines or vaccine candidates exist against these viral diseases, but all could potentially be improved if the immunogenicity of the vaccine could be enhanced. We found that the immunogenicity in primates of a live-attenuated vaccine candidate for parainfluenza virus type 3, an enveloped RNA virus that is an important etiologic agent of pediatric respiratory tract disease, could be enhanced by expression of granulocyte–macrophage colony-stimulating factor (GM-CSF) from an extra gene inserted into the genome of a cDNA-derived virus. Expression of GM-CSF by the live attenuated recombinant virus did not per se affect the level of pulmonary viral replication in rhesus monkeys after topical administration, which was 40-fold lower than that of WT parainfluenza virus type 3. Despite that, the expressed extra gene augmented the virus-specific serum antibody response to a level that was ( i ) 3- to 6-fold higher than that induced by the same virus with an unrelated RNA insert of equal length and ( ii ) equal to the response induced by nonattenuated WT virus. In addition, topical immunization with the attenuated virus expressing GM-CSF induced a greater number of virus-specific IFN-γ-secreting T lymphocytes in the peripheral blood of monkeys than did immunization with the control virus bearing an unrelated RNA insert. These findings show that the immunogenicity of a live-attenuated vaccine virus in primates can be enhanced without increasing the level of virus replication. Thus, it might be possible to develop live-attenuated vaccines that are as immunogenic as parental WT virus or, possibly, even more so.

Published

2002

16. Sendai Virus, a Murine Parainfluenza Virus Type 1, Replicates to a Level Similar to Human PIV1 in the Upper and Lower Respiratory Tract of African Green Monkeys and Chimpanzees

Author

Daniel Kolakofsky, Mario H. Skiadopoulos, Peter L. Collins, Brian R. Murphy, Marisa St. Claire, Machiko Nishio, William R. Elkins, Jeffrey M. Riggs, Sonja R. Surman, and Dominique Garcin

Subjects

Pan troglodytes, Respiratory System, Parainfluenza Virus 1, Human/immunology/physiology, Respirovirus Infections/immunology/prevention & control, Antibodies, Viral, Vaccines, Attenuated, Virus Replication, Respirovirus Infections, Sendai virus, Sendai virus/immunology/physiology, Species Specificity, Neutralization Tests, Virology, Chlorocebus aethiops, medicine, Animals, Antibodies, Viral/analysis, Vector (molecular biology), Viral Vaccines/administration & dosage, ddc:616, biology, Transmission (medicine), Pan troglodytes/virology, Viral Vaccines, biology.organism_classification, Parainfluenza Virus 1, Human, Disease Models, Animal, Human Parainfluenza Virus, medicine.anatomical_structure, Respiratory System/virology, Viral replication, Immunology, Viral disease, African Green Monkey, Cercopithecus aethiops/virology, Respiratory tract

Abstract

Human parainfluenza virus type 1 (HPIV1), a major cause of croup in infants and young children, accounts for 6% of hospitalizations for pediatric respiratory tract disease. The antigenically related Sendai virus, referred to here as murine PIV1 (MPIV1), is being considered for use as a live-attenuated vaccine to protect against HPIV1 (J. L. Hurwitz, K. F. Soike, M. Y., Sangster, A. Portner, R. E. Sealy, D. H. Dawson, and C. Coleclough, 1997, Vaccine 15(5), 533–540) and also as a recombinant vaccine vector expressing antigens to protect against viral disease in humans. However, in the 1950s MPIV1 was reported to have been isolated from humans, suggesting that zoonotic transmission might have occurred. It is therefore important to examine the ability of MPIV1 to replicate in nonhuman primates, i.e., surrogate hosts for humans. In the present study the level of replication of MPIV1 and HPIV1 was compared in African green monkeys and chimpanzees. Surprisingly, MPIV1 replicated as efficiently as HPIV1 in the upper and lower respiratory tract of African green monkeys at doses of 104 and 106 and replicated only slightly less efficiently at both sites in chimpanzees. African green monkeys immunized with MPIV1 were highly resistant to subsequent challenge with HPIV1 even though MPIV1 did not induce a detectable HPIV1-neutralizing antibody response. The high level of replication of MPIV1 observed in the upper and lower respiratory tract of these primates suggests that MPIV1 likely would require significant attenuation before it could be given to humans as a vaccine against HPIV1 or as a vaccine vector. Its ability to efficiently replicate in nonhuman primates suggests that MPIV1 lacks a significant host range restriction in primates and could theoretically cause zoonotic disease in humans.

Published

2002

17. Evaluation of the Replication and Immunogenicity of Recombinant Human Parainfluenza Virus Type 3 Vectors Expressing up to Three Foreign Glycoproteins

Author

Claes Örvell, Sonja R. Surman, Brian R. Murphy, Jeffrey M. Riggs, Mario H. Skiadopoulos, and Peter L. Collins

Subjects

Genetic Vectors, Gene Expression, Hemagglutinins, Viral, Hemagglutinin (influenza), Antibodies, Viral, Virus Replication, Insert (molecular biology), Virus, Cell Line, law.invention, Measles virus, Neutralization Tests, law, Cricetinae, Virology, Animals, Gene, HN Protein, biology, Viral Vaccines, Hemagglutination Tests, biology.organism_classification, Fusion protein, Parainfluenza Virus 3, Human, Viral replication, Drug Design, Recombinant DNA, biology.protein, Reassortant Viruses

Abstract

The level of replication and immunogenicity of recombinant parainfluenza virus type 3 (rHPIV3) bearing one, two, or three gene insertions expressing foreign protective antigens was examined. cDNA-derived recombinant HPIV3s bearing genes encoding the open reading frames (ORFs) of the hemagglutinin-neuraminidase (HN) of HPIV1, the HN of HPIV2, or the hemagglutinin (HA) of measles virus replicated efficiently in vitro, including the largest recombinant, which had three gene unit insertions and which was almost 23 kb in length, 50% longer than unmodified HPIV3. Several viruses were recovered from cDNAs whose genome length was not a multiple of six nucleotides and these contained nucleotide insertions that corrected the length to be a multiple of 6, confirming that the “rule of six” applies to HPIV3. Using a hemagglutination inhibition assay, we determined that the HPIV1 HN expressed by recombinant HPIV3 was incorporated into HPIV3 virions, whereas using this assay incorporation of the HPIV2 HN could not be detected. HPIV3 virions bearing HPIV1 HN were not neutralized by HPIV1 antiserum but were readily neutralized by antibodies to the HPIV3 HN or fusion protein (F). Viruses with inserts were restricted for replication in the respiratory tract of hamsters, and the level of restriction was a function of the total number of genes inserted, the nature of the insert, and the position of the inserted gene in the gene order. A single insert of HPIV2 HN or measles virus HA reduced the in vivo replication of rHPIV3 up to 25-fold, whereas the HPIV1 HN insert decreased replication almost 1000-fold. This indicates that the HPIV1 HN insert has an attenuating effect in addition to that of the extra gene insert itself, presumably because it is incorporated into the virus particle. Viruses containing two inserts were generally more attenuated than those with a single insert, and viruses with three inserts were over-attenuated for replication in hamsters. Inserts between the N and P genes were slightly more attenuating than those between the P and the M genes. A recombinant HPIV3 bearing both the HPIV1 and the HPIV2 HN genes (r1HN 2HN) was attenuated, immunogenic, and protected immunized hamsters from challenge with HPIV1, HPIV2, and HPIV3. Thus, it is possible to use a single HPIV vector expressing two foreign gene inserts to protect infants and young children from the severe lower respiratory tract disease caused by the three major human PIV pathogens.

Published

2002

18. [Untitled]

Author

Mario H. Skiadopoulos, Jason T. Newman, Peter L. Collins, Brian R. Murphy, Sonja R. Surman, Chris T. Hansen, and Jeffrey M. Riggs

Subjects

biology, Sequence analysis, Virulence, General Medicine, biology.organism_classification, Virology, Sendai virus, Virus, Reverse genetics, Plasmid, Complementary DNA, Genetics, Consensus sequence, Molecular Biology

Abstract

A complete consensus sequence was determined for the genomic RNA of human parainfluenza virus type 1 (HPIV1) strain Washington/20993/1964 (HPIV1 WASH/64), a clinical isolate that previously was shown to be virulent in adults. The sequence exhibited a high degree of relatedness to both Sendai virus, a PIV1 virus recovered from mice, and human PIV3 (HPIV3) with regard to cis-acting regulatory regions and protein-coding sequences. This consensus sequence was used to generate a full-length antigenomic cDNA and to recover a recombinant wild-type HPIV1 (rHPIV1). Interestingly, the rHPIV1 could be rescued from full-length antigenomic rHPIV1 cDNA using HPIV3 support plasmids, HPIV1 support plasmids, or a mixture thereof. The replication of rHPIV1 in vitro and in the respiratory tract of hamsters was similar to that of its biologically derived parent virus. The similar biological properties of rHPIV1 and HPIV1 WASH/64 in vitro and in vivo, together with the previous demonstration of the virulence of this specific isolate in humans, authenticates the rHPIV1 sequence as that of a wild-type virus. This rHPIV1 can now be used to study the biological properties of HPIV1 and as a substrate to introduce attenuating mutations for the generation of live-attenuated HPIV1 vaccine candidates.

Published

2002

19. A Chimeric Human-Bovine Parainfluenza Virus Type 3 Expressing Measles Virus Hemagglutinin Is Attenuated for Replication but Is Still Immunogenic in Rhesus Monkeys

Author

Brian R. Murphy, Peter L. Collins, Jeffrey M. Riggs, Sonja R. Surman, and Mario H. Skiadopoulos

Subjects

viruses, Measles Vaccine, Respiratory System, Immunology, Hemagglutinins, Viral, Antibodies, Viral, Vaccines, Attenuated, Virus Replication, Recombinant virus, Microbiology, Measles, Respirovirus, Virus, Measles virus, Virology, Vaccines and Antiviral Agents, medicine, Animals, Humans, Neutralizing antibody, Vaccines, Synthetic, biology, Chimera, Viral culture, biology.organism_classification, medicine.disease, Macaca mulatta, Parainfluenza Virus 3, Human, Insect Science, Respiratory Syncytial Virus Vaccines, biology.protein, Cattle, Immunization, Measles vaccine

Abstract

The chimeric recombinant virus rHPIV3-N B , a version of human parainfluenza virus type 3 (HPIV3) that is attenuated due to the presence of the bovine PIV3 nucleocapsid (N) protein open reading frame (ORF) in place of the HPIV3 ORF, was modified to encode the measles virus hemagglutinin (HA) inserted as an additional, supernumerary gene between the HPIV3 P and M genes. This recombinant, designated rHPIV3-N B HA, replicated like its attenuated rHPIV3-N B parent virus in vitro and in the upper and lower respiratory tracts of rhesus monkeys, indicating that the insertion of the measles virus HA did not further attenuate rHPIV3-N B in vitro or in vivo. Monkeys immunized with rHPIV3-N B HA developed a vigorous immune response to both measles virus and HPIV3, with serum antibody titers to both measles virus (neutralizing antibody) and HPIV3 (hemagglutination inhibiting antibody) of over 1:500. An attenuated HPIV3 expressing a major protective antigen of measles virus provides a method for immunization against measles by the intranasal route, a route that has been shown with HPIV3 and respiratory syncytial virus vaccines to be relatively refractory to the neutralizing and immunosuppressive effects of maternally derived virus-specific serum antibodies. It should now be possible to induce a protective immune response against measles virus in 6-month-old infants, an age group that in developing areas of the world is not responsive to the current measles virus vaccine.

Published

2001

20. Construction of a live-attenuated bivalent vaccine virus against human parainfluenza virus (PIV) types 1 and 2 using a recombinant PIV3 backbone

Author

Brian R. Murphy, Sonja R. Surman, Fatemeh Davoodi, Tao Tao, Mario H. Skiadopoulos, and Peter L. Collins

Subjects

Paramyxoviridae, Vaccines, Attenuated, Respirovirus Infections, Virus, Cell Line, law.invention, law, Cricetinae, Vaccines, DNA, Animals, Humans, Paramyxovirinae, HN Protein, Mononegavirales, Parainfluenza Vaccines, Vaccines, Synthetic, General Veterinary, General Immunology and Microbiology, biology, Public Health, Environmental and Occupational Health, Wild type, biology.organism_classification, Virology, Parainfluenza Virus 1, Human, Parainfluenza Virus 2, Human, Human Parainfluenza Virus, Infectious Diseases, Recombinant DNA, Molecular Medicine

Abstract

PIV1 and PIV2 are important agents of pediatric respiratory tract disease. We are developing live-attenuated vaccines against these viruses. We earlier constructed a PIV3/PIV1 antigenic chimeric virus, designated rPIV3-1, in which the hemagglutinin-neuraminidase (HN) and fusion (F) proteins of wild type rPIV3 were replaced by their PIV1 counterparts. In the present study, rPIV3-1 was used as a vector to express the HN protein of PIV2 to generate a single virus capable of inducing immunity to both PIV1 and PIV2. The PIV2 HN open reading frame was expressed from an extra gene cassette, under the control of PIV3 cis-acting transcription signals, inserted between the F and HN genes of rPIV3-1. The recombinant derivative, designated rPIV3-1.2HN, was readily recovered and exhibited a level of temperature sensitivity and in vitro growth similar to that of its parental virus. The rPIV3-1.2HN virus was restricted in replication in both the upper and lower respiratory tracts of hamsters compared with rPIV3-1, identifying an attenuating effect of the PIV2 HN insert in hamsters. rPIV3-1.2HN elicited serum antibodies to both PIV1 and PIV2 and induced resistance against challenge with wild type PIV1 or PIV2. Thus, rPIV3-1.2HN, a virus attenuated solely by the insertion of the PIV2 HN gene, functioned as a live attenuated bivalent vaccine candidate against both PIV1 and PIV2.

Published

2001

21. Comparison of Identical Temperature-Sensitive Mutations in the L Polymerase Proteins of Sendai and Parainfluenza3 Viruses

Author

Brian R. Murphy, Mario H. Skiadopoulos, Sue A. Moyer, Sherin Smallwood, and Joyce A. Feller

Subjects

Transcription, Genetic, viruses, Molecular Sequence Data, Mutant, RNA-dependent RNA polymerase, Respirovirus, Virus, 03 medical and health sciences, chemistry.chemical_compound, Transcription (biology), Virology, RNA polymerase, Humans, Amino Acid Sequence, Cells, Cultured, Polymerase, 030304 developmental biology, 0303 health sciences, biology, 030302 biochemistry & molecular biology, Temperature, RNA, DNA-Directed RNA Polymerases, biology.organism_classification, Molecular biology, Parainfluenza Virus 3, Human, 3. Good health, Protein Subunits, chemistry, Vesicular stomatitis virus, Mutation, biology.protein, RNA, Viral

Abstract

The L subunit of the RNA-dependent RNA polymerase of negative strand RNA viruses is believed to possess all the enzymatic activities necessary for viral transcription and replication. Mutations in the L proteins of human parainfluenza virus type 3 (PIV3) and vesicular stomatitis virus (VSV) have been shown to confer temperature sensitivity to the viruses; however, their specific defects have not been determined. Mutant PIV3 L proteins expressed from plasmids were tested for temperature sensitivity in transcription and replication in a minigenome reporter system in cells and for in vitro transcription from purified PIV3 template. The single L mutants, Y942H and L992F, were temperature sensitive (ts) in both assays, although viral RNA synthesis was not completely abolished at the nonpermissive temperature. Surprisingly, the T1558I L mutant was not ts, although its cognate virus was ts. Thus the ts defect in this virus may be due to the abrogation of an essential interaction of the mutant polymerase with a host cell component, which is not measured by the RNA synthesis assays. Most of the combinations of the PIV3 L mutations were not additive and did not show temperature sensitivity in in vitro transcription. Since they were ts in the minigenome assay in vivo, replication appears to be specifically defective. The ts mutations in PIV3 and VSV L proteins were also substituted into the Sendai L protein to compare the defects in related systems. Only Sendai Y942H L was ts in both transcription and replication. One Sendai L mutant, L992F, gave much better replication than transcription. Several other mutants could transcribe but not replicate in vitro, while replication in vivo was normal.

Published

2000

22. Human Parainfluenza Virus Type 3 (PIV3) Expressing the Hemagglutinin Protein of Measles Virus Provides a Potential Method for Immunization against Measles Virus and PIV3 in Early Infancy

Author

Jeffrey M. Riggs, Mario H. Skiadopoulos, Peter L. Collins, Brian R. Murphy, Josephine M. McAuliffe, Anna P. Durbin, and Sonja R. Surman

Subjects

viruses, Measles Vaccine, Molecular Sequence Data, Immunology, Hemagglutinins, Viral, Antibodies, Viral, Virus Replication, Microbiology, Measles, Virus, law.invention, Measles virus, law, Cricetinae, Virology, Vaccines and Antiviral Agents, medicine, Animals, Humans, Cells, Cultured, Vaccines, Synthetic, Base Sequence, Mesocricetus, biology, Vaccination, Temperature, Infant, biology.organism_classification, medicine.disease, Parainfluenza Virus 3, Human, Human Parainfluenza Virus, Titer, Insect Science, Recombinant DNA, biology.protein, Antibody

Abstract

Recombinant human parainfluenza virus type 3 (PIV3) was used as a vector to express the major protective antigen of measles virus, the hemagglutinin (HA) glycoprotein, in order to create a bivalent PIV3-measles virus that can be administered intranasally. The measles virus HA open reading frame (ORF) was inserted as an additional transcriptional unit into the N-P, P-M, or HA-neuraminidase (HN)-L gene junction of wild-type PIV3 or into the N-P or P-M gene junction of an attenuated derivative of PIV3, termed r cp 45L. The recombinant PIV3 (rPIV3) viruses bearing the HA inserts replicated more slowly in vitro than their parental viruses but reached comparable peak titers of ≥10 7.5 50% tissue culture infective doses per ml. Each of the wild-type or cold-passaged 45L ( cp 45L) PIV3(HA) chimeric viruses replicated 5- to 10-fold less well than its respective parent virus in the upper respiratory tract of hamsters. Thus, insertion of the ∼2-kb ORF itself conferred attenuation, and this attenuation was additive to that conferred by the cp 45L mutations. The attenuated cp 45L PIV3(HA) recombinants induced a high level of resistance to replication of PIV3 challenge virus in hamsters and induced very high levels of measles virus neutralizing antibodies (>1:8,000) that are well in excess of those known to be protective in humans. rPIV3s expressing the HA gene in the N-P or P-M junction induced about 400-fold more measles virus-neutralizing antibody than did the rPIV3 with the HA gene in the HN-L junction, indicating that the N-P or P-M junction appears to be the preferred insertion site. Previous studies indicated that the PIV3 cp 45 virus, a more attenuated version of r cp 45L, replicates efficiently in the respiratory tract of monkeys and is immunogenic and protective even when administered in the presence of very high titers of passively transferred PIV3 antibodies (A. P. Durbin, C. J. Cho, W. R. Elkins, L. S. Wyatt, B. Moss, and B. R. Murphy, J. Infect. Dis. 179:1345–1351, 1999). This suggests that this intranasally administered PIV3(HA) chimeric virus can be used to immunize infants with maternally acquired measles virus antibodies in whom the current parenterally administered live measles virus vaccine is ineffective.

Published

2000

23. Replacement of the Ectodomains of the Hemagglutinin-Neuraminidase and Fusion Glycoproteins of Recombinant Parainfluenza Virus Type 3 (PIV3) with Their Counterparts from PIV2 Yields Attenuated PIV2 Vaccine Candidates

Author

Fatemeh Davoodi, Tao Tao, Mario H. Skiadopoulos, Brian R. Murphy, Jeffrey M. Riggs, and Peter L. Collins

Subjects

Pan troglodytes, Molecular Sequence Data, Respiratory System, Immunology, Biology, Vaccines, Attenuated, Virus Replication, Microbiology, Cell Line, law.invention, Parainfluenza virus type 2, law, Cricetinae, Virology, Chlorocebus aethiops, Vaccines and Antiviral Agents, Animals, Amino Acid Sequence, HN Protein, Vero Cells, Recombination, Genetic, Vaccines, Synthetic, Base Sequence, Mesocricetus, Viral Vaccine, Vaccination, Viral Vaccines, Parainfluenza Virus 2, Human, Parainfluenza Virus 3, Human, Protein Structure, Tertiary, Transmembrane domain, Viral replication, Ectodomain, Insect Science, Mutagenesis, Site-Directed, Recombinant DNA, Viral Fusion Proteins, Hemagglutinin-neuraminidase

Abstract

We sought to develop a live attenuated parainfluenza virus type 2 (PIV2) vaccine strain for use in infants and young children, using reverse genetic techniques that previously were used to rapidly produce a live attenuated PIV1 vaccine candidate. The PIV1 vaccine candidate, designated rPIV3-1cp45, was generated by substituting the full-length HN and F proteins of PIV1 for those of PIV3 in the attenuated cp 45 PIV3 vaccine candidate (T. Tao et al., J. Virol. 72:2955–2961, 1998; M. H. Skiadopoulos et al., Vaccine 18:503–510, 1999). However, using the same strategy, we failed to recover recombinant chimeric PIV3-PIV2 isolate carrying the full-length PIV2 glycoproteins in a wild-type PIV3 backbone. Viable PIV3-PIV2 chimeras were recovered when chimeric HN and F open reading frames (ORFs) rather than complete PIV2 F and HN ORFs were used to construct the full-length cDNA. The recovered viruses, designated rPIV3-2CT, in which the PIV2 ectodomain and transmembrane domain were fused to the PIV3 cytoplasmic domain, and rPIV3-2TM, in which the PIV2 ectodomain was fused to the PIV3 transmembrane and cytoplasmic tail domain, possessed similar in vitro and in vivo phenotypes. Thus, it appeared that only the cytoplasmic tail of the HN or F glycoprotein of PIV3 was required for successful recovery of PIV3-PIV2 chimeras. Although rPIV3-2CT and rPIV3-2TM replicated efficiently in vitro, they were moderately to highly attenuated for replication in the respiratory tracts of hamsters, African green monkeys (AGMs), and chimpanzees. This unexpected finding indicated that chimerization of the HN and F proteins of PIV2 and PIV3 itself specified an attenuation phenotype in vivo. Despite this attenuation, these viruses were highly immunogenic and protective against challenge with wild-type PIV2 in hamsters and AGMs, and they represent promising candidates for clinical evaluation as a vaccine against PIV2. These chimeric viruses were further attenuated by the addition of 12 mutations of PIV3cp45 which lie outside of the HN and F genes. The attenuating effects of these mutations were additive with that of the chimerization, and thus inclusion of all or some of the cp 45 mutations provides a means to further attenuate the PIV3-PIV2 chimeric vaccine candidates if necessary.

Published

2000

24. A live attenuated recombinant chimeric parainfluenza virus (PIV) candidate vaccine containing the hemagglutinin-neuraminidase and fusion glycoproteins of PIV1 and the remaining proteins from PIV3 induces resistance to PIV1 even in animals immune to PIV3

Author

Mario H. Skiadopoulos, Fatemah Davoodi, Tao Tao, Chris J. Cho, Brian R. Murphy, Peter L. Collins, and Anna P. Durbin

Subjects

Paramyxoviridae, Recombinant Fusion Proteins, Neuraminidase, Cross immunity, Vaccines, Attenuated, Recombinant virus, Respirovirus Infections, Virus, Immunity, Cricetinae, Animals, Mononegavirales, Vaccines, Synthetic, Mesocricetus, General Veterinary, General Immunology and Microbiology, biology, Public Health, Environmental and Occupational Health, Viral Vaccines, biology.organism_classification, Virology, Fusion protein, Parainfluenza Virus 1, Human, Parainfluenza Virus 2, Human, Parainfluenza Virus 3, Human, Hemagglutinins, Infectious Diseases, Evaluation Studies as Topic, Molecular Medicine, Immunization, Viral Fusion Proteins, Hemagglutinin-neuraminidase

Abstract

Using a reverse genetics system for PIV3, we previously recovered recombinant chimeric PIV3-PIV1 virus bearing the major protective antigens of PIV1, the hemaglutinin-neuraminidase and fusion proteins, on a background of PIV3 genes bearing temperature sensitive (ts) and attenuating mutations in the L gene. Immunization of hamsters with this virus, designated rPIV3-1.cp45L, induced a high level of resistance to replication of wild type (wt) PIV1 and, surprisingly, also induced a moderate amount of restriction of the replication of PIV3 challenge virus. This suggested that some immunity is conferred by the internal PIV3 proteins shared by the two viruses. In the present study, we found that the immunity to PIV3 conferred by infection with rPIV3-1.cp45L is short-lived and completely disappeared four months after immunization, whereas resistance to replication of PIV3 induced by prior infection with PIV3 remains high even after an interval of four months. Since a live attenuated PIV1 vaccine such as the chimeric rPIV3-1.cp45L virus will likely be given to infants after a live attenuated PIV3 vaccine in a sequential immunization schedule, we examined the immunogenicity and efficacy of rPIV3-1.cp45L against PIV1 challenge in animals with and without prior immunity to PIV3. rPIV3-1.cp45L efficiently infected hamsters previously infected with wt or attenuated PIV3, but there was approximately a five-fold reduction in replication of rPIV3-1. cp45L virus in the PIV3-immune animals. This reduction in replication of rPIV3-1.cp45L in PIV3-immune animals was accompanied by a significant decrease in efficacy against PIV1 challenge. However, rPIV3-1.cp45L immunization of PIV3-immune animals induced a vigorous serum antibody response to PIV1 and reduced replication of PIV1 challenge virus 1000-fold in the lower respiratory tract and 25 to 200-fold in the upper respiratory tract. This study demonstrated that the recombinant chimeric rPIV3-1.cp45L candidate vaccine can induce immunity to PIV1 even in animals immune to PIV3. This establishes the feasibility of employing a sequential immunization schedule in which a recombinant chimeric rPIV3-1.cp45L vaccine is given following a live attenuated PIV3 vaccine.

Published

2000

25. [Untitled]

Author

Jane E. Bailly, Brian R. Murphy, Mario H. Skiadopoulos, Peter L. Collins, and Josephine M. McAuliffe

Subjects

Genetics, Viral matrix protein, Strain (chemistry), General Medicine, Biology, Virology, Phenotype, Genome, Reverse genetics, Human Parainfluenza Virus, Phosphoprotein, Molecular Biology, Peptide sequence

Abstract

The Kansas/15626/84 (Ka) and Shipping Fever (SF) strains of bovine parainfluenza virus type 3 (BPIV3) replicate less efficiently than human PIV3 (HPIV3) in the upper and lower respiratory tract of rhesus monkeys, and BPIV3 Ka is also highly attenuated in humans and is in clinical trials as a candidate vaccine against HPIV3. To initiate an investigation of the genetic basis of the observed attenuation phenotype of BPIV3 in primates, the complete genomic sequences of Ka and SF genomes were determined and compared to those of BPIV3 strain 910N and two HPIV3 strains, JS and Wash/47885/57. There is a high degree of identity between the five PIV3 viruses in their 55 nucleotide (nt) leader (83.6%) and 44 nt trailer (93.2%) sequences. The five viruses display amino acid sequence identity ranging from 58.6% for the phosphoprotein to 89.7% for the matrix protein. Interestingly, the majority of amino acid residues found to be variable at a given position in a five-way protein alignment are nonetheless identical within the viruses of either host species (BPIV3 or HPIV3). These host-specific residues might be products of distinct selective pressures on BPIV3 and HPIV3 during evolution in their respective hosts. These host-specific sequences likely include ones which are responsible for the host range differences, such as the efficient growth of BPIV3 in bovines compared to its restricted growth in primates. It should now be possible using the techniques of reverse genetics to import sequences from BPIV3 into HPIV3 and identify those nt or protein sequences which attenuate HPIV3 for primates. This information should be useful in understanding virus-host interactions and in the development of vaccines to protect against HPIV3-induced disease.

Published

2000

26. Identification of Mutations Contributing to the Temperature-Sensitive, Cold-Adapted, and Attenuation Phenotypes of the Live-Attenuated Cold-Passage 45 ( cp 45) Human Parainfluenza Virus 3 Candidate Vaccine

Author

Anna P. Durbin, Brian R. Murphy, Shin Lu Wu, Maribel Paschalis, Sonja R. Surman, Peter L. Collins, Mario H. Skiadopoulos, Stephen A. Udem, and Joanne M. Tatem

Subjects

Immunology, Adaptation, Biological, Viral Plaque Assay, Biology, Vaccines, Attenuated, Recombinant virus, Microbiology, Virus, Cell Line, law.invention, law, Cricetinae, Virology, Vaccines and Antiviral Agents, Animals, Humans, Gene, Virus quantification, Genetics, Point mutation, Viral Vaccines, Macaca mulatta, Molecular biology, Phenotype, Reverse genetics, Parainfluenza Virus 3, Human, Cold Temperature, Insect Science, Mutation, Recombinant DNA

Abstract

The live-attenuated human parainfluenza virus 3 (PIV3) cold-passage 45 ( cp 45) candidate vaccine was shown previously to be safe, immunogenic, and phenotypically stable in seronegative human infants. Previous findings indicated that each of the three amino acid substitutions in the L polymerase protein of cp 45 independently confers the temperature-sensitive ( ts ) and attenuation ( att ) phenotypes but not the cold-adaptation ( ca ) phenotype (29). cp 45 contains 12 additional potentially important point mutations in other proteins (N, C, M, F, and hemagglutinin-neuraminidase [HN]) or in cis -acting sequences (the leader region and the transcription gene start [GS] signal of the N gene), and their contribution to these phenotypes was undefined. To further characterize the genetic basis for the ts , ca , and att phenotypes of this promising vaccine candidate, we constructed, using a reverse genetics system, a recombinant cp 45 virus that contained all 15 cp 45-specific mutations mentioned above, and found that it was essentially indistinguishable from the biologically derived cp 45 on the basis of plaque size, level of temperature sensitivity, cold adaptation, level of replication in the upper and lower respiratory tract of hamsters, and ability to protect hamsters from subsequent wild-type PIV3 challenge. We then constructed recombinant viruses containing the cp 45 mutations in individual proteins as well as several combinations of mutations. Analysis of these recombinant viruses revealed that multiple cp 45 mutations distributed throughout the genome contribute to the ts , ca , and att phenotypes. In addition to the mutations in the L gene, at least one other mutation in the 3′ N region (i.e., including the leader, N GS, and N coding changes) contributes to the ts phenotype. A recombinant virus containing all the cp 45 mutations except those in L was more ts than cp 45, illustrating the complex nature of this phenotype. The ca phenotype of cp 45 also is a complex composite phenotype, reflecting contributions of at least three separate genetic elements, namely, mutations within the 3′ N region, the L protein, and the C-M-F-HN region. The att phenotype is a composite of both ts and non- ts mutations. Attenuating ts mutations are located in the L protein, and non- ts attenuating mutations are located in the C and F proteins. The presence of multiple ts and non- ts attenuating mutations in cp 45 likely contributes to the high level of attenuation and phenotypic stability of this promising vaccine candidate.

Published

1999

27. Three Amino Acid Substitutions in the L Protein of the Human Parainfluenza Virus Type 3 cp 45 Live Attenuated Vaccine Candidate Contribute to Its Temperature-Sensitive and Attenuation Phenotypes

Author

Peter L. Collins, Anna P. Durbin, Shin Lu Wu, Brian R. Murphy, Maribel Paschalis, Joanne M. Tatem, Mario H. Skiadopoulos, and Tao Tao

Subjects

Immunology, Mutant, Mutagenesis (molecular biology technique), Viral Plaque Assay, Biology, Vaccines, Attenuated, Recombinant virus, Microbiology, Virus, Cell Line, law.invention, Viral Proteins, law, Cricetinae, Virology, Animal Viruses, Tumor Cells, Cultured, Animals, Humans, Gene, chemistry.chemical_classification, Genetics, Attenuated vaccine, Mesocricetus, Temperature, Viral Vaccines, DNA-Directed RNA Polymerases, Macaca mulatta, Molecular biology, Parainfluenza Virus 3, Human, Amino acid, Phenotype, chemistry, Insect Science, Mutagenesis, Site-Directed, Recombinant DNA

Abstract

Studies were initiated to define the genetic basis of the temperature-sensitive ( ts ), cold adaptation ( ca ), and attenuation ( att ) phenotypes of the human parainfluenza virus type 3 (PIV3) cp 45 live attenuated vaccine candidate. Genetic data had previously suggested that the L polymerase protein of cp 45, which contains three amino acid substitutions at positions 942, 992, and 1558, contributed to its temperature sensitivity (R. Ray, M. S. Galinski, B. R. Heminway, K. Meyer, F. K. Newman, and R. B. Belshe, J. Virol. 70:580–584, 1996; A. Stokes, E. L. Tierney, C. M. Sarris, B. R. Murphy, and S. L. Hall, Virus Res. 30:43–52, 1993). To study the individual and aggregate contributions that these amino acid substitutions make to the ts , att , and ca phenotypes of cp 45, seven PIV3 recombinant viruses (three single, three double, and one triple mutant) representing all possible combinations of the three amino acid substitutions were recovered from full-length antigenomic cDNA and analyzed for their ts , att , and ca phenotypes. None of the seven mutant recombinant PIVs was cold adapted. The substitutions at L protein amino acid positions 992 and 1558 each specified a 10 5 -fold reduction in plaque formation in cell culture at 40°C, whereas the substitution at position 942 specified a 300-fold reduction. Thus, each of the three mutations contributes individually to the ts phenotype. The triple recombinant which possesses an L protein with all three mutations was almost as temperature sensitive as cp 45, indicating that these mutations are the major contributors to the ts phenotype of cp 45. The three individual mutations in the L protein each contributed to restricted replication in the upper or lower respiratory tract of hamsters, and this likely contributes to the observed stability of the ts and att phenotypes of cp 45 during replication in vivo. Importantly, the recombinant virus possessing L protein with all three mutations was as restricted in replication as was the cp 45 mutant in both the upper and lower respiratory tracts of hamsters, indicating that the L gene of the cp 45 virus is a major attenuating component of this candidate vaccine.

Published

1998

28. Bovine Papillomavirus Type 1 Genomes and the E2 Transactivator Protein Are Closely Associated with Mitotic Chromatin

Author

Alison A. McBride and Mario H. Skiadopoulos

Subjects

Cell division, viruses, Antigens, Polyomavirus Transforming, Immunology, Mitosis, CHO Cells, Genome, Viral, Biology, Microbiology, DNA-binding protein, Genome, Cell Line, Viral Proteins, Transactivation, Cricetinae, Virology, Chlorocebus aethiops, Tumor Cells, Cultured, Animals, Bovine papillomavirus 1, Sequence Deletion, Bovine papillomavirus, DNA replication, biology.organism_classification, Molecular biology, Chromatin, Virus-Cell Interactions, DNA-Binding Proteins, Insect Science, COS Cells, DNA, Viral, Trans-Activators, Cattle

Abstract

The bovine papillomavirus type 1 E2 transactivator protein is required for viral transcriptional regulation and DNA replication and may be important for long-term episomal maintenance of viral genomes within replicating cells (M. Piirsoo, E. Ustav, T. Mandel, A. Stenlund, and M. Ustav, EMBO J. 15:1–11, 1996). We have evidence that, in contrast to most other transcriptional transactivators, the E2 transactivator protein is associated with mitotic chromosomes in dividing cells. The shorter E2-TR and E8/E2 repressor proteins do not bind to mitotic chromatin, and the N-terminal transactivation domain of the E2 protein is necessary for the association. However, the DNA binding function of E2 is not required. We have found that bovine papillomavirus type 1 genomes are also associated with mitotic chromosomes, and we propose a model in which E2-bound viral genomes are transiently associated with cellular chromosomes during mitosis to ensure that viral genomes are segregated to daughter cells in approximately equal numbers.

Published

1998

29. Effect of Anthrax Immune Globulin on Response to BioThrax (Anthrax Vaccine Adsorbed) in New Zealand White Rabbits

Author

Nina V. Malkevich, Mario H. Skiadopoulos, Gary S. Nabors, Boris Ionin, Kristin H. Clement, Ronald T. Aimes, Ajoy C. Chakrabarti, Subhendu Basu, and Thomas L. Rudge

Subjects

Male, Anthrax Vaccines, Biology, complex mixtures, Anthrax, Antigen, Animals, Humans, Pharmacology (medical), Experimental Therapeutics, Infusions, Intravenous, Respiratory Tract Infections, Pharmacology, Anthrax vaccines, Anthrax immune globulin, fungi, Vaccination, Anthrax Vaccine Adsorbed, Immunoglobulins, Intravenous, biology.organism_classification, bacterial infections and mycoses, Virology, Antibodies, Bacterial, Bacillus anthracis, Infectious Diseases, Immunization, Area Under Curve, Immunology, biology.protein, Female, Rabbits, Antibody, Drug Antagonism, Half-Life

Abstract

Development of anthrax countermeasures that may be used concomitantly in a postexposure setting requires an understanding of the interaction between these products. Anthrax immune globulin intravenous (AIGIV) is a candidate immunotherapeutic that contains neutralizing antibodies against protective antigen (PA), a component of anthrax toxins. We evaluated the interaction between AIGIV and BioThrax (anthrax vaccine adsorbed) in rabbits. While pharmacokinetics of AIGIV were not altered by vaccination, the vaccine-induced immune response was abrogated in AIGIV-treated animals.

Published

2013

30. Mutational Analysis of Conserved Tyrosines in the NS-1 Protein of the Parvovirus Minute Virus of Mice

Author

Emmanuel A. Faust and Mario H. Skiadopoulos

Subjects

DNA Replication, Transcriptional Activation, Phenylalanine, DNA polymerase II, DNA Mutational Analysis, Molecular Sequence Data, Eukaryotic DNA replication, Viral Nonstructural Proteins, Biology, Transfection, DNA replication factor CDT1, Structure-Activity Relationship, Replication factor C, Control of chromosome duplication, Virology, Animals, Amino Acid Sequence, Replication protein A, Cells, Cultured, Base Sequence, Sequence Homology, Amino Acid, DNA replication, Molecular biology, Minute Virus of Mice, Mutagenesis, Site-Directed, biology.protein, Tyrosine, Origin recognition complex

Abstract

The NS-1 gene of the parvovirus minute virus of mice encodes a multifunctional protein essential for viral DNA replication and gene expression. In addition to possessing DNA helicase and ATPase activities, NS-1 forms a covalent linkage with the 5′ ends of viral DNA and is a strong candidate for the site-specific nicking-closing enzyme postulated to be involved in the resolution of concatemers and terminal hairpin structures that arise during parvoviral DNA replication. Since the covalent linkage between NS-1 and the 5′ terminus of MVM DNA resists alkali and mild acid treatment, a tyrosine phosphodiester is likely to be involved. To map domains responsible for this activity, mutations converting tyrosine to phenylalanine were introduced into the NS-1 gene using oligonucleotide-directed mutagenesis and their effect on the DNA replication and transcriptional activation functions of NS-1 was examined in transient in vivo transfection assays. Replacement of Tyr-188, Tyr-197, Tyr-210, Tyr-310, Tyr-422, or Tyr-550 with phenylalanine greatly reduced the ability of NS-1 to complement the replication of the target genome ins 20B in COS-7 cells. However, a Ser-545 to Thr-545 substitution in the Phe-550 mutant restored DNA replication activity. Replacement of 5 other tyrosines in NS-1 with phenylalanine either enhanced (Phe-6), had a moderate inhibitory effect (Phe-209) or had no effect (Phe-47, Phe 227 and Phe-543) on its DNA replication activity. Two of the 11 phenylalanine substitution mutations, Phe-188 and Phe-197, also greatly reduced the ability of NS-1 to transactivate the p38 promoter and displayed a dominant negative phenotype with respect to transactivation. Since the remaining tyrosines in MVM NS-1, Tyr-152, Tyr-252, Tyr-374, and Tyr-595, are not conserved among the NS-1 proteins encoded by porcine and feline parvoviruses, they are presumed to be nonessential for the normal functioning of NS-1. The results point to a role for either Tyr-188, Tyr-197, Tyr-210, Tyr-310, or Tyr-422 in forming a covalent linkage with viral DNA and further suggest a regulatory role for several tyrosines in other DNA replication and transcriptional activation functions of NS-1.

Published

1993

31. Role of Interferon in the Replication of Human Parainfluenza Virus Type 1 Wild Type and Mutant Viruses in Human Ciliated Airway Epithelium

Author

Mario H. Skiadopoulos, Brian R. Murphy, Peter L. Collins, Raymond J. Pickles, Alexander C. Schmidt, Margaret Hennessey, and Emmalene J. Bartlett

Subjects

Paramyxoviridae, Immunology, Alpha interferon, Cellular Response to Infection, Bronchi, Microbiology, Models, Biological, Virus, Interferon, Virology, medicine, Humans, Cilia, Mononegavirales, Microscopy, Confocal, biology, Reverse Transcriptase Polymerase Chain Reaction, Wild type, Temperature, Interferon-alpha, Interferon-beta, biology.organism_classification, Parainfluenza Virus 1, Human, Protein Structure, Tertiary, Trachea, Human Parainfluenza Virus, Phenotype, Insect Science, Mutation, Respiratory epithelium, Interferons, medicine.drug

Abstract

Human parainfluenza virus type 1 (HPIV1) is a significant cause of pediatric respiratory disease in the upper and lower airways. An in vitro model of human ciliated airway epithelium (HAE), a useful tool for studying respiratory virus-host interactions, was used in this study to show that HPIV1 selectively infects ciliated cells within the HAE and that progeny virus is released from the apical surface with little apparent gross cytopathology. In HAE, type I interferon (IFN) is induced following infection with an HPIV1 mutant expressing defective C proteins with an F170S amino acid substitution, rHPIV1-C F170S , but not following infection with wild-type HPIV1. IFN induction coincided with a 100- to 1,000-fold reduction in virus titer, supporting the hypothesis that the HPIV1 C proteins are critical for the inhibition of the innate immune response. Two recently characterized live attenuated HPIV1 vaccine candidates expressing mutant C proteins were also evaluated in HAE. The vaccine candidates, rHPIV1-C R84G/Δ170 HN T553A L Y942A and rHPIV1-C R84G/Δ170 HN T553A L Δ1710-11 , which contain temperature-sensitive ( ts ) attenuating ( att ) and non- ts att mutations, were highly restricted in growth in HAE at permissive (32°C) and restrictive (37°C) temperatures. The viruses grew slightly better at 37°C than at 32°C, and rHPIV1-C R84G/Δ170 HN T553A L Y942A was less attenuated than rHPIV1-C R84G/Δ170 HN T553A L Δ1710-11 . The level of replication in HAE correlated with that previously observed for African green monkeys, suggesting that the HAE model has potential as a tool for the preclinical evaluation of HPIV1 vaccines, although how these in vitro data will correlate with vaccine virus replication in seronegative human subjects remains to be seen.

Published

2008

32. Modification of the trypsin-dependent cleavage activation site of the human metapneumovirus fusion protein to be trypsin independent does not increase replication or spread in rodents or nonhuman primates

Author

Mario H. Skiadopoulos, Ursula J. Buchholz, Stéphane Biacchesi, Quynh N. Pham, Brian R. Murphy, and Peter L. Collins

Subjects

medicine.medical_treatment, Immunology, Cleavage (embryo), Virus Replication, Microbiology, Human metapneumovirus, Virology, Cricetinae, Chlorocebus aethiops, medicine, Disease Transmission, Infectious, Animals, Metapneumovirus, Trypsin, Amino Acid Sequence, Furin, Protease, Binding Sites, biology, biology.organism_classification, Fusion protein, Viral replication, Insect Science, Mutation, biology.protein, Pathogenesis and Immunity, Immunization, Viral Fusion Proteins, medicine.drug

Abstract

The contribution of cleavage activation of the fusion F protein of human metapneumovirus (HMPV) to replication and pathogenicity in rodents and nonhuman primates was investigated. Recombinant HMPVs were generated in which the naturally occurring trypsin-dependent cleavage sequence (R-Q-S-R↓) was replaced by each of three sequences whose cleavage in vitro does not depend upon added trypsin. Two of these were multibasic sequences derived from avian metapneumovirus type A (R-R-R-R) or type C (R-K-A-R), with the former containing the consensus furin protease cleavage motif (R-X-R/K-R↓). The third one (R-Q-P-R) was derived from a recently described trypsin independent HMPV isolate (J. H. Schickli, J. Kaur, N. Ulbrandt, R. R. Spaete, and R. S. Tang, J. Virol. 79: 10678-10689, 2005). To preclude the possibility of conferring even greater virulence to this significant human pathogen, the modifications were done in an HMPV variant that was attenuated by the deletion of two of the three envelope glycoproteins, SH and G. Each of the introduced cleavage sequences conferred trypsin independent F cleavage and growth to HMPV in vitro. However, they differed in the efficiency of trypsin independent growth and plaque formation in vitro: R-R-R-R > R-K-A-R > R-Q-P-R > R-Q-S-R. The R-R-R-R mutant was the only one whose growth in vitro was not augmented by added trypsin, indicative of highly efficient trypsin independent cleavage. When inoculated intranasally into hamsters, there was essentially no difference in the magnitude of replication in the upper or lower respiratory tract between the mutants, and virus was not detected in organs outside of the respiratory tract. Evaluation of the most cleavage-efficient mutant, R-R-R-R, in African green monkeys showed that there was no detectable change in the magnitude of replication in the upper and lower respiratory tract or in immunogenicity and protective efficacy against HMPV challenge. These results suggest that cleavage activation is not a major determinant of HMPV virulence.

Published

2006

33. Chimeric Recombinant Human Metapneumoviruses with the Nucleoprotein or Phosphoprotein Open Reading Frame Replaced by That of Avian Metapneumovirus Exhibit Improved Growth In Vitro and Attenuation In Vivo

Author

Quynh N. Pham, Peter L. Collins, Ursula J. Buchholz, Mario H. Skiadopoulos, Stéphane Biacchesi, and Brian R. Murphy

Subjects

Genes, Viral, viruses, Recombinant Fusion Proteins, Immunology, Virus Replication, Microbiology, Chimera (genetics), Open Reading Frames, Human metapneumovirus, Virology, Cricetinae, Vaccines and Antiviral Agents, Chlorocebus aethiops, Animals, Humans, Metapneumovirus, Vero Cells, Recombination, Genetic, biology, Virulence, Immunogenicity, virus diseases, Viral Vaccines, biology.organism_classification, Phosphoproteins, Nucleoprotein, respiratory tract diseases, Titer, Nucleoproteins, Viral replication, Insect Science, Vero cell, Gene Deletion

Abstract

Chimeric versions of recombinant human metapneumovirus (HMPV) were generated by replacing the nucleoprotein (N) or phosphoprotein (P) open reading frame with its counterpart from the closely related avian metapneumovirus (AMPV) subgroup C. In Vero cells, AMPV replicated to an approximately 100-fold-higher titer than HMPV. Surprisingly, the N and P chimeric viruses replicated to a peak titer that was 11- and 25-fold higher, respectively, than that of parental HMPV. The basis for this effect is not known but was not due to obvious changes in the efficiency of gene expression. AMPV and the N and P chimeras were evaluated for replication, immunogenicity, and protective efficacy in hamsters. AMPV was attenuated compared to HMPV in this mammalian host on day 5 postinfection, but not on day 3, and only in the nasal turbinates. In contrast, the N and P chimeras were reduced approximately 100-fold in both the upper and lower respiratory tract on day 3 postinfection, although there was little difference by day 5. The N and P chimeras induced a high level of neutralizing serum antibodies and protective efficacy against HMPV; AMPV was only weakly immunogenic and protective against HMPV challenge, reflecting antigenic differences. In African green monkeys immunized intranasally and intratracheally, the mean peak titer of the P chimera was reduced 100- and 1,000-fold in the upper and lower respiratory tracts, whereas the N chimera was reduced only 10-fold in the lower respiratory tract. Both chimeras were comparable to wild-type HMPV in immunogenicity and protective efficacy. Thus, the P chimera is a promising live HMPV vaccine candidate that paradoxically combines improved growth in vitro with attenuation in vivo.

Published

2005

34. Introducing point and deletion mutations into the P/C gene of human parainfluenza virus type 1 (HPIV1) by reverse genetics generates attenuated and efficacious vaccine candidates

Author

Sonja R. Surman, Emerito Amaro-Carambot, Emmalene J. Bartlett, Mario H. Skiadopoulos, Brian R. Murphy, and Peter L. Collins

Subjects

Paramyxoviridae, Biology, medicine.disease_cause, Vaccines, Attenuated, Virus, Cell Line, Interferon, Cricetinae, medicine, Animals, Humans, Point Mutation, Mononegavirales, Parainfluenza Vaccines, Mutation, General Veterinary, General Immunology and Microbiology, Point mutation, Public Health, Environmental and Occupational Health, Wild type, biology.organism_classification, Virology, Reverse genetics, Parainfluenza Virus 1, Human, Infectious Diseases, Molecular Medicine, medicine.drug

Abstract

The P/C gene of human parainfluenza virus type 1 (HPIV1) encodes a nested set of related accessory C proteins, C′/C/Y1/Y2, which have been shown in other paramyxoviruses to have a role in evasion of the type I interferon (IFN) response following virus infection. We previously demonstrated that a set of two amino acid substitutions, C R84G /HN T553A , and a separate amino acid substitution, C F170S , are independently attenuating for HPIV1 in African green monkeys (AGMs). However, in each case the attenuation ( att ) phenotype is vulnerable to reversion by a single nucleotide change back to wild type. Using reverse genetics, recombinant HPIV1 (rHPIV1) vaccine candidates were generated that were designed for increased genetic and phenotypic stability by: (i) creating a two-amino acid deletion and substitution at the site of the C F170S mutation, yielding C Δ170 ; (ii) introducing a six amino acid deletion in the N-terminal region of C, C Δ10–15 ; and (iii) combining these stable deletion mutations with the att C R84G /HN T553A mutation. The resulting rHPIV1 vaccine candidates were evaluated for attenuation in hamsters and AGMs and for immunogenicity and protective efficacy in AGMs. The C Δ10–15 mutation was attenuating in hamsters but not in AGMs, and likely will be of limited value for an HPIV1 vaccine. Conversely, the C R84G /HN T553A mutation set was attenuating in AGMs but not in hamsters. Thus, these two mutations demonstrated reciprocal host range phenotypes involving different regions of C. The C Δ170 mutation conferred a significant level of attenuation in hamsters and AGMs that closely resembled that of C F170S and will be of particular utility for vaccine development because it involves a deletion of six nucleotides rendering it highly refractory to reversion. The combination of the C R84G /HN T553A mutation set and the C Δ170 deletion mutation yielded a virus, rC R84G/Δ170 HN T553A , that exhibited a satisfactory level of attenuation in hamsters and AGMs and was immunogenic and highly protective against HPIV1 wt challenge. This virus will be evaluated clinically as a live intranasal HPIV1 vaccine, one that can be further attenuated as necessary by the introduction of additional stabilized att mutations previously developed in the L protein.

Published

2005

35. Deletion of M2 Gene Open Reading Frames 1 and 2 of Human Metapneumovirus: Effects on RNA Synthesis, Attenuation, and Immunogenicity

Author

Lijuan Yang, Brian R. Murphy, Stéphane Biacchesi, Kim C. Tran, Quynh N. Pham, Peter L. Collins, Cindy Luongo, Mario H. Skiadopoulos, and Ursula J. Buchholz

Subjects

Genes, Viral, viruses, Immunology, Molecular Sequence Data, Biology, Virus Replication, Microbiology, Virus, Viral Matrix Proteins, Open Reading Frames, Viral Proteins, Human metapneumovirus, Virology, Cricetinae, Vaccines and Antiviral Agents, Chlorocebus aethiops, Animals, Humans, Metapneumovirus, Amino Acid Sequence, Gene, Vero Cells, Recombination, Genetic, Paramyxoviridae Infections, Base Sequence, Mesocricetus, Virulence, Immunogenicity, virus diseases, Viral Vaccines, biology.organism_classification, respiratory tract diseases, Open reading frame, Viral replication, Insect Science, DNA, Viral, Vero cell, RNA, Viral, Gene Deletion

Abstract

The M2 gene of human metapneumovirus (HMPV) contains two overlapping open reading frames (ORFs), M2-1 and M2-2. The expression of separate M2-1 and M2-2 proteins from these ORFs was confirmed, and recombinant HMPVs were recovered in which expression of M2-1 and M2-2 was ablated individually or together [rΔM2-1, rΔM2-2, and rΔM2(1+2)]. Each M2 mutant virus directed efficient multicycle growth in Vero cells. The ability to recover HMPV lacking M2-1 contrasts with human respiratory syncytial virus, for which M2-1 is an essential transcription factor. Expression of the downstream HMPV M2-2 ORF was not reduced when translation of the upstream M2-1 ORF was silenced, indicating that it is initiated separately. The rΔM2-2 mutants exhibited a two- to fivefold increase in the accumulation of mRNA, normalized to the genome template, suggesting that M2-2 has a role in regulating RNA synthesis. Replication and immunogenicity were tested in hamsters. Animals infected intranasally with rΔM2-1 or rΔM2(1+2) did not have recoverable virus in the lungs or nasal turbinates on days 3 or 5 postinfection and did not develop HMPV-neutralizing serum antibodies or resistance to HMPV challenge. Thus, M2-1 appears to be essential for significant virus replication in vivo. In animals infected with rΔM2-2, virus was recovered from only 1 of 12 animals and only in the nasal turbinates on a single day. However, all of the animals developed a high titer of HMPV-neutralizing serum antibodies and were highly protected against challenge with wild-type HMPV. The HMPV rΔM2-2 virus is a promising and highly attenuated HMPV vaccine candidate.

Published

2005

36. Rapid human metapneumovirus microneutralization assay based on green fluorescent protein expression

Author

Stéphane Biacchesi, Brian R. Murphy, Ursula J. Buchholz, Lijuan Yang, Mario H. Skiadopoulos, and Peter L. Collins

Subjects

Time Factors, Serial dilution, Green Fluorescent Proteins, Biology, biology.organism_classification, Antibodies, Viral, Virology, Molecular biology, Recombinant Proteins, Incubation period, Green fluorescent protein, Cell Line, Titer, Human metapneumovirus, Neutralization Tests, Chlorocebus aethiops, Vero cell, Microneutralization Assay, Animals, Humans, Metapneumovirus, Vero Cells

Abstract

We describe a simple and expedited microneutralization assay for human metapneumovirus virus (HMPV) based on a recombinant HMPV expressing the enhanced green fluorescent protein (rHMPV-GFP). Test serum dilutions were incubated with fixed amounts of rHMPV-GFP and inoculated onto Vero cells, and the growth of non-neutralized rHMPV-GFP was visualized by fluorescent microscopy of living cells. A preliminary titer could be determined following 3 days of incubation. GFP expression was sufficient to be read by an automated scanner after 4-5 days of incubation, which also provided a permanent record. In comparison, the conventional serum neutralization assay requires a longer incubation time plus the additional steps of fixation and staining or immunostaining. rHMPV-GFP-based titers could be determined by the 50% infectivity endpoint method of Reed and Muench [Reed, L.J., Muench, H., 1938. A simple method of estimating fifty per cent endpoint. Am. J. Hyg. 27, 493-497], or by automated scanning and non-linear regression to determine the 50% endpoint of GFP fluorescence. The latter method was two- to three-fold more sensitive. This assay also permits automation and up-scaling, making it suitable for broad HMPV seroepidemiology studies and experiments that require large scale serology, such as vaccine studies.

Published

2005

37. Recombinant Human Metapneumovirus Lacking the Small Hydrophobic SH and/or Attachment G Glycoprotein: Deletion of G Yields a Promising Vaccine Candidate

Author

Mario H. Skiadopoulos, Elaine W. Lamirande, Lijuan Yang, Brian R. Murphy, Peter L. Collins, Ursula J. Buchholz, Kim C. Tran, and Stéphane Biacchesi

Subjects

G protein, viruses, Immunology, Biology, medicine.disease_cause, Virus Replication, Microbiology, Virus, Viral Proteins, Human metapneumovirus, Viral Envelope Proteins, Virology, Cricetinae, Vaccines and Antiviral Agents, medicine, Animals, Metapneumovirus, HN Protein, Recombination, Genetic, Mutation, Mesocricetus, Viral Vaccine, Viral Vaccines, biology.organism_classification, Viral replication, Insect Science, RNA, Viral, Gene Deletion

Abstract

Human metapneumovirus (HMPV) has recently been identified as a significant cause of serious respiratory tract disease in humans. In particular, the emerging information on the contribution of HMPV to pediatric respiratory tract disease suggests that it will be important to develop a vaccine against this virus for use in conjunction with those being developed for human respiratory syncytial virus and the human parainfluenza viruses. A recently described reverse genetic system (S. Biacchesi, M. H. Skiadopoulos, K. C. Tran, B. R. Murphy, P. L. Collins, and U. J. Buchholz, Virology 321:247-259, 2004) was used to generate recombinant HMPVs (rHMPVs) that lack the G gene, the SH gene, or both. The ΔSH, ΔG, and ΔSH/G deletion mutants were readily recovered and were found to replicate efficiently during multicycle growth in cell culture. Thus, the SH and G proteins are not essential for growth in cell culture. Apart from the absence of the deleted protein(s), the virions produced by the gene deletion mutants were similar by protein yield and gel electrophoresis protein profile to wild-type HMPV. When administered intranasally to hamsters, the ΔG and ΔSH/G mutants replicated in both the upper and lower respiratory tracts, showing that HMPV containing F as the sole viral surface protein is competent for replication in vivo. However, both viruses were at least 40-fold and 600-fold restricted in replication in the lower and upper respiratory tract, respectively, compared to wild-type rHMPV. They also induced high titers of HMPV-neutralizing serum antibodies and conferred complete protection against replication of wild-type HMPV challenge virus in the lungs. Surprisingly, G is dispensable for protection, and the ΔG and ΔSH/G viruses represent promising vaccine candidates. In contrast, ΔSH replicated somewhat more efficiently in hamster lungs compared to wild-type rHMPV (20-fold increase on day 5 postinfection). This indicates that SH is completely dispensable in vivo and that its deletion does not confer an attenuating effect, at least in this rodent model.

Published

2004

38. Human parainfluenza virus type I (HPIV1) vaccine candidates designed by reverse genetics are attenuated and efficacious in African green monkeys

Author

Jason T. Newman, Sonja R. Surman, Mario H. Skiadopoulos, Brian R. Murphy, Peter L. Collins, Emerito Amaro-Carambot, and Emmalene J. Bartlett

Subjects

Biology, medicine.disease_cause, Antibodies, Viral, Vaccines, Attenuated, Respirovirus Infections, Virus, law.invention, Viral Proteins, law, medicine, Animals, Humans, Point Mutation, Parainfluenza Vaccines, Mutation, General Veterinary, General Immunology and Microbiology, Immunogenicity, Public Health, Environmental and Occupational Health, Temperature, Virology, Macaca mulatta, Reverse genetics, Parainfluenza Virus 1, Human, Human Parainfluenza Virus, Disease Models, Animal, Infectious Diseases, Recombinant DNA, Molecular Medicine, Nasal administration, African Green Monkey

Abstract

A set of recombinant, live attenuated human parainfluenza virus type 1 (rHPIV1) vaccine candidates was evaluated for attenuation, immunogenicity, and protective efficacy in African green monkeys (AGMs). Temperature sensitive (ts) and non-ts attenuating (att) mutations in the P/C and L genes were introduced individually or in various combinations into rHPIV1, including the C(R84G) and HN(T553A) mutations identified in the present work and the C(F170S), L(Y942A), and L(L992C) mutations identified previously. The rHPIV1 vaccine candidates exhibited a spectrum of attenuation in AGMs. One genetically and phenotypically stable vaccine candidate, rC(R84G/F170S)L(Y942A/L992C), was attenuated and efficacious in AGMs and is a promising live attenuated intranasal HPIV1 vaccine candidate suitable for clinical evaluation.

Published

2004

39. The two major human metapneumovirus genetic lineages are highly related antigenically, and the fusion (F) protein is a major contributor to this antigenic relatedness

Author

Josephine M. McAuliffe, Stéphane Biacchesi, Brian R. Murphy, William R. Elkins, Ursula J. Buchholz, Mario H. Skiadopoulos, Peter L. Collins, Marisa St. Claire, Jeffrey M. Riggs, Sonja R. Surman, and Emerito Amaro-Carambot

Subjects

Pan troglodytes, viruses, Immunology, Molecular Sequence Data, Respiratory System, Heterologous, Cross Reactions, Antibodies, Viral, Virus Replication, Microbiology, Neutralization, Virus, Epitope, Cell Line, Human metapneumovirus, Neutralization Tests, Virology, Cricetinae, Antigenic variation, Animals, Humans, Metapneumovirus, Paramyxoviridae Infections, biology, Base Sequence, virus diseases, biology.organism_classification, Antigenic Variation, respiratory tract diseases, Parainfluenza Virus 1, Human, Disease Models, Animal, Insect Science, biology.protein, Pathogenesis and Immunity, Antibody, Viral Fusion Proteins

Abstract

The growth properties and antigenic relatedness of the CAN98-75 (CAN75) and the CAN97-83 (CAN83) human metapneumovirus (HMPV) strains, which represent the two distinct HMPV genetic lineages and exhibit 5 and 63% amino acid divergence in the fusion (F) and attachment (G) proteins, respectively, were investigated in vitro and in rodents and nonhuman primates. Both strains replicated to high titers (≥6.0 log 10 ) in the upper respiratory tract of hamsters and to moderate titers (≥3.6 log 10 ) in the lower respiratory tract. The two lineages exhibited 48% antigenic relatedness based on reciprocal cross-neutralization assay with postinfection hamster sera, and infection with each strain provided a high level of resistance to reinfection with the homologous or heterologous strain. Hamsters immunized with a recombinant human parainfluenza virus type 1 expressing the fusion F protein of the CAN83 strain developed a serum antibody response that efficiently neutralized virus from both lineages and were protected from challenge with either HMPV strain. This result indicates that the HMPV F protein is a major antigenic determinant that mediates extensive cross-lineage neutralization and protection. Both HMPV strains replicated to low titers in the upper and lower respiratory tracts of rhesus macaques but induced high levels of HMPV-neutralizing antibodies in serum effective against both lineages. The level of HMPV replication in chimpanzees was moderately higher, and infected animals developed mild colds. HMPV replicated the most efficiently in the respiratory tracts of African green monkeys, and the infected animals developed a high level of HMPV serum-neutralizing antibodies (1:500 to 1:1,000) effective against both lineages. Reciprocal cross-neutralization assays in which postinfection sera from all three primate species were used indicated that CAN75 and CAN83 are 64 to 99% related antigenically. HMPV-infected chimpanzees and African green monkeys were highly protected from challenge with the heterologous HMPV strain. Taken together, the results from hamsters and nonhuman primates support the conclusion that the two HMPV genetic lineages are highly related antigenically and are not distinct antigenic subtypes or subgroups as defined by reciprocal cross-neutralization in vitro.

Published

2004

40. Codon Substitution Mutations at Two Positions in the L Polymerase Protein of Human Parainfluenza Virus Type 1 Yield Viruses with a Spectrum of Attenuation In Vivo and Increased Phenotypic Stability In Vitro

Author

Brian R. Murphy, Sonja R. Surman, Peter L. Collins, Jason T. Newman, Mario H. Skiadopoulos, Josephine M. McAuliffe, and Jeffrey M. Riggs

Subjects

Silent mutation, Immunology, Mutant, Respiratory System, DNA-Directed DNA Polymerase, medicine.disease_cause, Vaccines, Attenuated, Virus Replication, Microbiology, Respirovirus Infections, Cell Line, Viral Proteins, Serial passage, Virology, Cricetinae, Vaccines and Antiviral Agents, medicine, Missense mutation, Animals, Humans, Codon, Parainfluenza Vaccines, Polymerase, Genetics, Mutation, biology, Temperature, Molecular biology, Parainfluenza Virus 1, Human, Phenotype, Amino Acid Substitution, Insect Science, Codon usage bias, biology.protein, Synonymous substitution

Abstract

The Y942H and L992F temperature-sensitive ( ts ) and attenuating amino acid substitution mutations, previously identified in the L polymerase of the HPIV3 cp 45 vaccine candidate, were introduced into homologous positions of the L polymerase of recombinant human parainfluenza virus type 1 (rHPIV1). In rHPIV1, the Y942H mutation specified the ts phenotype in vitro and the attenuation ( att ) phenotype in hamsters, whereas the L992F mutation specified neither phenotype. Each of these codon mutations was generated by a single nucleotide substitution and therefore had the potential to readily revert to a codon specifying the wild-type amino acid residue. We introduced alternative amino acid assignments at codon 942 or 992 as a strategy to increase genetic stability and to generate mutants that exhibit a range of attenuation. Twenty-three recombinants with codon substitutions at position 942 or 992 of the L protein were viable. One highly ts and att mutant, the Y942A virus, which had a difference of three nucleotides from the codon encoding a wild-type tyrosine, also possessed a high level of genetic and phenotypic stability upon serial passage in vitro at restrictive temperatures compared to that of the parent Y942H virus, which possessed a single nucleotide substitution. We obtained mutants with substitutions at position 992 that, in contrast to the L992F virus, possessed the ts and att phenotypes. These findings identify the use of alternative codon substitution mutations as a method that can be used to generate candidate vaccine viruses with increased genetic stability and/or a modified level of attenuation.

Published

2004

41. Generation of recombinant human parainfluenza virus type 1 vaccine candidates by importation of temperature-sensitive and attenuating mutations from heterologous paramyxoviruses

Author

Jason T. Newman, Sonja R. Surman, Mario H. Skiadopoulos, Jeffrey M. Riggs, Teresa A. Mulaikal, Josephine M. McAuliffe, Peter L. Collins, and Brian R. Murphy

Subjects

Paramyxoviridae, Immunology, Mutant, Molecular Sequence Data, Heterologous, Biology, Recombinant virus, medicine.disease_cause, Antibodies, Viral, Vaccines, Attenuated, Microbiology, Respirovirus Infections, Virus, Viral Proteins, Virology, Cricetinae, Vaccines and Antiviral Agents, medicine, Animals, Humans, Point Mutation, Mononegavirales, Parainfluenza Vaccines, Mutation, Vaccines, Synthetic, Base Sequence, Mesocricetus, Point mutation, Temperature, biology.organism_classification, Parainfluenza Virus 1, Human, Parainfluenza Virus 3, Human, Respiratory Syncytial Viruses, Insect Science

Abstract

Human parainfluenza virus type 1 (HPIV1) is a significant cause of respiratory tract disease in infants and young children for which a vaccine is needed. In the present study, we sought to attenuate HPIV1 by the importation of one or more known attenuating point mutations from heterologous paramyxoviruses into homologous sites in HPIV1. The introduced mutations were derived from three attenuated paramyxoviruses: (i) HPIV3 cp 45, a live-attenuated HPIV3 vaccine candidate containing multiple attenuating mutations; (ii) the respiratory syncytial virus cpts 530 with an attenuating mutation in the L polymerase protein; and (iii) a murine PIV1 (MPIV1) attenuated by a mutation in the accessory C protein. Recombinant HPIV1 (rHPIV1) mutants bearing a single imported mutation in C, any of three different mutations in L, or a pair of mutations in F exhibited a 100-fold or greater reduction in replication in the upper or lower respiratory tract of hamsters. Both temperature-sensitive ( ts ) (mutations in the L and F proteins) and non- ts (the mutation in the C protein) attenuating mutations were identified. rHPIV1 mutants containing a combination of mutations in L were generated that were more attenuated than viruses bearing the individual mutations, showing that the systematic accretion of mutations can yield progressive increases in attenuation. Hamsters immunized with rHPIV1 mutants bearing one or two mutations developed neutralizing antibodies and were resistant to challenge with wild-type HPIV1. Thus, importation of attenuating mutations from heterologous viruses is an effective means for rapidly identifying mutations that attenuate HPIV1 and for generating live-attenuated HPIV1 vaccine candidates.

Published

2004

42. Genetic diversity between human metapneumovirus subgroups

Author

Guy Boivin, Brian R. Murphy, Mario H. Skiadopoulos, Stéphane Biacchesi, Ursula J. Buchholz, Christopher T. Hanson, and Peter L. Collins

Subjects

viruses, Molecular Sequence Data, Genome, Virus, Genomic sequence, Cell Line, Open Reading Frames, Viral Proteins, Human metapneumovirus, Virology, Genotype, Humans, Metapneumovirus, Amino Acid Sequence, Peptide sequence, Genetics, Genetic diversity, biology, Base Sequence, Nucleic acid sequence, virus diseases, Genetic Variation, Sequence Analysis, DNA, biology.organism_classification, respiratory tract diseases, Subgroup

Abstract

Complete consensus nucleotide sequences were determined for human metapneumovirus (HMPV) isolates CAN97-83 and CAN98-75, representing the two proposed genotypes or genetic subgroups of HMPV. The overall level of genome nucleotide sequence identity and aggregate proteome amino acid sequence identity between the two HMPV subgroups were 80 and 90%, respectively, similar to the respective values of 81 and 88% between the two antigenic subgroups of human respiratory syncytial virus (HRSV). The diversity between HMPV subgroups was greatest for the SH and G proteins (59 and 37% identity, respectively), which were even more divergent than their HRSV counterparts (72 and 55% cross-subgroup identity, respectively). It is reasonable to anticipate that the two genetic subgroups of HMPV represent antigenic subgroups approximately comparable to those of HRSV.

Published

2003

43. The Genome Length of Human Parainfluenza Virus Type 2 Follows the Rule of Six, and Recombinant Viruses Recovered from Non-Polyhexameric-Length Antigenomic cDNAs Contain a Biased Distribution of Correcting Mutations

Author

Sonja R. Surman, Mario H. Skiadopoulos, Brian R. Murphy, Jeffrey M. Riggs, Leatrice Vogel, and Peter L. Collins

Subjects

Paramyxoviridae, Immunology, Molecular Sequence Data, Replication, Context (language use), Genome, Viral, Biology, Microbiology, Genome, law.invention, Intergenic region, law, Virology, Complementary DNA, Chlorocebus aethiops, Animals, Amino Acid Sequence, Gene, Vero Cells, Genetics, Recombination, Genetic, Base Sequence, Reverse Transcriptase Polymerase Chain Reaction, biology.organism_classification, Parainfluenza Virus 2, Human, Viral replication, Insect Science, Mutation, Recombinant DNA

Abstract

Members of the Paramyxovirinae subfamily of the Paramyxoviridae family of viruses have the unusual requirement that the nucleotide length of the viral genome must be an even multiple of six in order for efficient RNA replication, and hence virus replication, to occur. Human parainfluenza virus type 2 (HPIV2) is the only member of the genus that has been reported to have a genome length that is not an even multiple of six, and it has also been recovered from a full-length antigenomic-sense cDNA that did not conform to the “rule of six.” To reexamine the issue of nucleotide length in natural isolates of HPIV2, a complete consensus genomic sequence was determined for three HPIV2 strains: Greer, Vanderbilt/1994 (V94), and Vanderbilt/1998. Each of these strains was found to have a genome length of 15,654 nucleotides (nt), thus conforming in each case to the rule of six. To directly examine the requirement that the genomic length of HPIV2 be an even multiple of six, we constructed six full-length antigenomic HPIV2/V94 cDNAs that deviated from a polyhexameric length by 0 to 5 nt. Recombinant HPIV2s were readily recovered from all of the cDNAs, including those that did not conform to the rule of six. One recombinant HPIV2 isolate was completely sequenced for each of the nonpolyhexameric antigenomic cDNAs. These were found to contain small nucleotide insertions or deletions that conferred polyhexameric length to the recovered genome. Interestingly, almost all of the length corrections occurred within the hemagglutinin-neuraminidase and large polymerase genes or the intervening intergenic region and thus were proximal to the insert that caused the deviation from the rule of six. These results demonstrate, in the context of complete infectious virus, that HPIV2 has a strong and seemingly absolute requirement for a polyhexameric genome.

Published

2003

44. The recombinant chimeric human parainfluenza virus type 1 vaccine candidate, rHPIV3-1cp45, is attenuated, immunogenic, and protective in African green monkeys

Author

Brian R. Murphy, Shin Lu Wu, Sonja R. Surman, William R. Elkins, Yvonne Mitcho, Joanne M. Tatem, and Mario H. Skiadopoulos

Subjects

Paramyxoviridae, Recombinant virus, Antibodies, Viral, Vaccines, Attenuated, Virus Replication, Respirovirus Infections, Virus, law.invention, law, Chlorocebus aethiops, Animals, Humans, Paramyxovirinae, Mononegavirales, Parainfluenza Vaccines, Vaccines, Synthetic, General Veterinary, General Immunology and Microbiology, biology, Chimera, Immunogenicity, Public Health, Environmental and Occupational Health, Temperature, biology.organism_classification, Virology, Parainfluenza Virus 1, Human, Human Parainfluenza Virus, Infectious Diseases, Mutation, Recombinant DNA, Molecular Medicine

Abstract

A recombinant live-attenuated chimeric human parainfluenza virus type 1 (HPIV1) candidate vaccine was previously generated by replacing the fusion (F) and hemagglutinin-neuraminidase (HN) glycoprotein open reading frames (ORFs) of the HPIV3 candidate vaccine, rHPIV3 cp 45, with those of wild-type HPIV1. Previously, this recombinant chimeric virus, designated rHPIV3–1 cp 45, exhibited a greater level of the temperature sensitivity of replication in vitro and a greater level of attenuation of replication in the respiratory tract of immunized hamsters when compared to its HPIV3 cp 45 parent virus. In the present study, rHPIV3–1 cp 45 was evaluated for its level of attenuation and efficacy in African green monkeys ( Cercopithecus aethiops ), a primate in which both HPIV1 and HPIV3 wild-type viruses replicate efficiently. The rHPIV3–1 cp 45 candidate vaccine was as restricted in replication in the upper and lower respiratory tract as its thoroughly characterized rHPIV3 cp 45 parent indicating that the attenuating mutations present in the rHPIV3 cp 45 backbone specified an appropriate level of attenuation of rHPIV3–1 cp 45 for primates. The level to which rHPIV3–1 cp 45 replicated in the respiratory tract of African green monkeys was also sufficient to induce a strong immune response to HPIV1 and provided protection against challenge with wild-type HPIV1. These results provide a basis for further evaluation of this HPIV1 candidate vaccine in humans.

Published

2002

45. Bovine parainfluenza virus type 3 (BPIV3) fusion and hemagglutinin-neuraminidase glycoproteins make an important contribution to the restricted replication of BPIV3 in primates

Author

Sonja R. Surman, William R. Elkins, Anne Huang, Mario H. Skiadopoulos, Josephine M. McAuliffe, Alexander C. Schmidt, Jane E. Bailly, Peter L. Collins, and Brian R. Murphy

Subjects

Primates, Immunology, Biology, Simian, Virus Replication, Microbiology, Virus, Respirovirus, law.invention, Cell Line, law, Virology, Vaccines and Antiviral Agents, Animals, Humans, Gene, chemistry.chemical_classification, HN Protein, biology.organism_classification, Nucleoprotein, Viral replication, chemistry, Insect Science, Recombinant DNA, Cattle, Glycoprotein, Hemagglutinin-neuraminidase, Viral Fusion Proteins

Abstract

This study examines the contribution of the fusion (F) and hemagglutinin-neuraminidase (HN) glycoprotein genes of bovine parainfluenza virus type 3 (BPIV3) to its restricted replication in the respiratory tract of nonhuman primates. A chimeric recombinant human parainfluenza type 3 virus (HPIV3) containing BPIV3 F and HN glycoprotein genes in place of its own and the reciprocal recombinant consisting of BPIV3 bearing the HPIV3 F and HN genes (rBPIV3-F H HN H ) were generated to assess the effect of glycoprotein substitution on replication of HPIV3 and BPIV3 in the upper and lower respiratory tract of rhesus monkeys. The chimeric viruses were readily recovered and replicated in simian LLC-MK2 cells to a level comparable to that of their parental viruses, suggesting that the heterologous glycoproteins were compatible with the PIV3 internal proteins. HPIV3 bearing the BPIV3 F and HN genes was restricted in replication in rhesus monkeys to a level similar to that of its BPIV3 parent virus, indicating that the glycoprotein genes of BPIV3 are major determinants of its host range restriction of replication in rhesus monkeys. rBPIV3-F H HN H replicated in rhesus monkeys to a level intermediate between that of HPIV3 and BPIV3. This observation indicates that the F and HN genes make a significant contribution to the overall attenuation of BPIV3 for rhesus monkeys. Furthermore, it shows that BPIV3 sequences outside the F and HN region also contribute to the attenuation phenotype in primates, a finding consistent with the previous demonstration that the nucleoprotein coding sequence of BPIV3 is a determinant of its attenuation for primates. Despite its restricted replication in the respiratory tract of rhesus monkeys, rBPIV3-F H HN H conferred a level of protection against challenge with HPIV3 that was indistinguishable from that induced by previous infection with wild-type HPIV3. The usefulness of rBPIV3-F H HN H as a vaccine candidate against HPIV3 and as a vector for other viral antigens is discussed.

Published

2000

46. Generation of a parainfluenza virus type 1 vaccine candidate by replacing the HN and F glycoproteins of the live-attenuated PIV3 cp45 vaccine virus with their PIV1 counterparts

Author

Sonja R. Surman, Mario H. Skiadopoulos, Tao Tao, Brian R. Murphy, and Peter L. Collins

Subjects

Paramyxoviridae, Respiratory System, Biology, Recombinant virus, Vaccines, Attenuated, Virus Replication, Virus, Cricetinae, Animals, Mononegavirales, Vaccines, Synthetic, Attenuated vaccine, HN Protein, General Veterinary, General Immunology and Microbiology, Mesocricetus, Public Health, Environmental and Occupational Health, Wild type, Viral Vaccines, biology.organism_classification, Virology, Parainfluenza Virus 1, Human, Infectious Diseases, Viral replication, Molecular Medicine, Viral Fusion Proteins

Abstract

Parainfluenza virus type 1 (PIV1) is a major cause of croup in infants and young children, and a vaccine is needed to prevent the serious disease caused by this virus. In the present study, a live attenuated PIV1 vaccine candidate was generated by modification of the extensively-studied PIV3 cold-passaged (cp) cp45 vaccine candidate using the techniques of reverse genetics. The HN and F glycoproteins of the PIV3 cp45 candidate vaccine virus were replaced with those of PIV1. This created a live attenuated PIV1 vaccine candidate, termed rPIV3-1 cp45, which contained the attenuated background of the PIV3 cp45 vaccine virus together with the HN and F protective antigens of PIV1. Three of the 15 mutations of cp45 lie within the HN and F genes, and those in the F gene are attenuating. Thus, some attenuation might be lost by the HN and F glycoprotein replacement. To address this issue we also constructed a derivative of PIV3 cp45, designated rPIV3 cp45 (F(wt)HN(wt)), that possessed wild type PIV3 HN and F glycoproteins but retained the 12 other cp45 mutations. rPIV3 cp45 (F(wt)HN(wt)) replicated in the respiratory tract of hamsters to a level three- to four-fold higher than rPIV3 cp45, indicating that loss of the two attenuating mutations in the cp45 F gene effected a slight reduction in the overall attenuation of cp45 for hamsters. However, the chimeric rPIV3-1 cp45 virus was about 5-fold more restricted in replication in hamsters than rPIV3 cp45 and about 15- to 20-fold more restricted than rPIV3 cp45 (F(wt)HN(wt)). This suggests that two components contribute to the attenuation of the new chimeric rPIV3-1 cp45 PIV1 vaccine candidate: one being the 12 cp45 mutations, which provide most of the observed attenuation, and the other resulting from the introduction of the heterologous PIV1 HN and F proteins into PIV3 (i.e., a chimerization effect). rPIV3-1 cp45 was observed to be immunogenic and protective against challenge with wild type PIV1 in hamsters. This virus shows sufficient promise that it should be evaluated further as a candidate live attenuated vaccine strain for preventing severe lower respiratory tract PIV1 disease in infants and young children.

Published

1999

47. A live attenuated chimeric recombinant parainfluenza virus (PIV) encoding the internal proteins of PIV type 3 and the surface glycoproteins of PIV type 1 induces complete resistance to PIV1 challenge and partial resistance to PIV3 challenge

Author

Anna P. Durbin, Brian R. Murphy, Mario H. Skiadopoulos, Fatemah Davoodi, Tao Tao, and Peter L. Collins

Subjects

Paramyxoviridae, Surface Properties, Respiratory System, Hemagglutinin Glycoproteins, Influenza Virus, Recombinant virus, Vaccines, Attenuated, Virus Replication, Virus, law.invention, Cell Line, law, Cricetinae, Animals, Humans, Mononegavirales, chemistry.chemical_classification, General Veterinary, General Immunology and Microbiology, biology, Mesocricetus, Public Health, Environmental and Occupational Health, Wild type, Temperature, biology.organism_classification, Virology, Parainfluenza Virus 1, Human, Parainfluenza Virus 3, Human, Human Parainfluenza Virus, Infectious Diseases, chemistry, Recombinant DNA, Molecular Medicine, Receptors, Virus, Immunization, Glycoprotein, Viral Fusion Proteins

Abstract

The recovery of wild type and attenuated human parainfluenza type 3 (PIV3) recombinant viruses has made possible a new strategy to rapidly generate a live-attenuated vaccine virus for PIV1. We previously replaced the coding sequences for the hemagglutinin-neuraminidase (HN) and fusion (F) proteins of PIV3 with those of PIV1 in the PIV3 antigenomic cDNA. This was used to recover a fully-viable, recombinant chimeric PIV3-PIV1 virus, termed rPIV3-1, which bears the major protective antigens of PIV1 and is wild type-like with regard to growth in cell culture and in hamsters [Tao T, Durbin AP, Whitehead SS, Davoodi F, Collins PL, Murphy BR. Recovery of a fully viable chimeric human parainfluenza virus (PIV) type 3 in which the hemagglutinin-neuraminidase and fusion glycoprotein have been replaced by those of PIV type 1. J Virol 1998;72:2955–2961]. Here we report the recovery of a derivative of rPIV3-1 carrying the three temperature-sensitive and attenuating amino acid coding changes found in the L gene of the live-attenuated cp45 PIV3 candidate vaccine virus. This virus, termed rPIV3-1.cp45L, is temperature-sensitive with a shut-off temperature of 38°C, which is similar to that of the recombinant rPIV3cp45L, which possesses the same three mutations. rPIV3-1.cp45L is attenuated in the respiratory tract of hamsters to the same extent as rPIV3cp45L. Infection of hamsters with rPIV3-1.cp45L generated a moderate level of hemagglutination-inhibiting antibodies against wild type PIV1 and induced complete resistance to challenge with wild type PIV1. This demonstrates that this novel attenuated chimeric virus is capable of inducing a highly effective immune response against PIV1. It confirms previous observations that the surface glycoproteins of parainfluenza viruses are sufficient to induce a high level of resistance to homologous virus challenge. Unexpectedly, infection with recombinant chimeric virus rPIV3-1.cp45L or rPIV3-1, each bearing the surface glycoprotein genes of PIV1 and the internal genes of PIV3, also induced a moderate level of resistance to replication of wild type PIV3 challenge virus. This indicates that the internal genes of PIV3 can independently induce protective immunity against PIV3 in rodents, albeit a lower level of resistance than that induced by the surface glycoproteins. Thus, a reverse genetics system for PIV3 has been used successfully to produce a live attenuated PIV1 vaccine candidate that is attenuated and protective in experimental infection in hamsters.

Published

1999

48. The bovine papillomavirus type 1 E2 transactivator and repressor proteins use different nuclear localization signals

Author

Mario H. Skiadopoulos and Andalison A. Mcbride

Subjects

Signal peptide, Recombinant Fusion Proteins, Immunology, Molecular Sequence Data, Repressor, Biology, Protein Sorting Signals, Microbiology, Cell Line, Transactivation, Viral Proteins, Transcription (biology), Virology, Animals, Amino Acid Sequence, Fluorescent Antibody Technique, Indirect, Bovine papillomavirus, Bovine papillomavirus 1, Sequence Deletion, Cell Nucleus, Binding Sites, DNA replication, Biological Transport, biology.organism_classification, Subcellular localization, beta-Galactosidase, Molecular biology, Cell biology, DNA-Binding Proteins, Repressor Proteins, Insect Science, Trans-Activators, Cattle, Peptides, Nuclear localization sequence, Research Article

Abstract

The E2 gene of bovine papillomavirus type 1 encodes at least three nuclear phosphoproteins that regulate viral transcription and DNA replication. All three proteins have a common C-terminal domain that has DNA-binding and dimerization activities. A basic region in this domain forms an alpha helix which makes direct contact with the DNA target. In this study, it is shown that in addition to its role in DNA binding, this basic region functions as a nuclear localization signal both in the E2 DNA-binding domain and in a heterologous protein. Deletion of this signal sequence resulted in increased accumulation of the E2 transactivator and repressor proteins in the cytoplasm, but nuclear localization was not eliminated. In the full-length transactivator protein, another signal, present in the N-terminal transactivation domain, is used for transport to the nucleus, and the C-terminal nuclear localization signal(s) are masked. The use of different nuclear localization signals could potentially allow differential regulation of the subcellular localization of the E2 transactivator and repressor proteins at some stage in the viral life cycle.

Published

1996

49. Characterization of linker insertion and point mutations in the NS-1 gene of minute virus of mice: effects on DNA replication and transcriptional activation functions of NS-1

Author

Mario H. Skiadopoulos, Wey Liang Leong, Ralph Salvino, and Emmanuel A. Faust

Subjects

DNA Replication, Gene Expression Regulation, Viral, Transcription, Genetic, Blotting, Western, Molecular Sequence Data, Restriction Mapping, Eukaryotic DNA replication, Viral Nonstructural Proteins, Transfection, Cell Line, DNA replication factor CDT1, Mice, Replication factor C, Capsid, Control of chromosome duplication, Virology, Animals, Amino Acid Sequence, Cloning, Molecular, Promoter Regions, Genetic, Replication protein A, biology, Base Sequence, Viral Core Proteins, Ter protein, Genetic Complementation Test, DNA replication, Molecular biology, Mutagenesis, Insertional, Phenotype, DNA, Viral, Mutation, biology.protein, Minute Virus of Mice, Mutagenesis, Site-Directed, Trans-Activators, Origin recognition complex

Abstract

The NS-1 gene of minute virus of mice encodes a multifunctional protein required for replication of the viral genome and for transcriptional regulation of the two MVM promoters. To study the localization of activities required for DNA replication and transactivation of the capsid gene promoter, insertion and point mutations were introduced into the NS-1 gene. The mutant NS-1 genes were expressed in COS-7 cells by using an SV 40 promoter driven NS-1 expression vector. The ability of the mutant proteins to complement a replication defective NS-1 mutant of the infectious MVM plasmid pMM984 and to activate transcription from the capsid gene promoter in chloramphenicol acetyl transferase expression assays was determined. Two point mutations Ser-249 to Ala and Lys-250 to Gin and a one amino acid insertion between Asp-606 and Leu-607 had no effect on viral DNA replication and transactivation activities. Six independent insertions of between 2 and 12 amino acids inhibited the DNA replication activity of NS-1 between 20-and at least 100-fold. There was no apparent correlation between the extent of inhibition of parvoviral DNA replication and the location of the mutations. The transcriptional activation function of NS-1 was inhibited between 1.5- and at least 20-fold and was therefore overall relatively less sensitive to mutagenesis than was its DNA replication function. An exception to this was a 5 amino acid insertion between Tyr-543 and Gin-544 that abolished transactivation as well as the ability of NS-1 to complement viral DNA replication.

Published

1992

50. Two spatially distinct genetic elements constitute a bipartite DNA replication origin in the minute virus of mice genome

Author

Emmanuel A. Faust, C R Astell, Mario H. Skiadopoulos, P Tam, R O Shade, and R Salvino

Subjects

DNA Replication, Models, Molecular, Genes, Viral, Immunology, Molecular Sequence Data, Restriction Mapping, Eukaryotic DNA replication, Biology, Pre-replication complex, Origin of replication, Transfection, Microbiology, Cell Line, Replication factor C, Control of chromosome duplication, Virology, Animals, Repetitive Sequences, Nucleic Acid, Genetics, Base Sequence, Genetic Complementation Test, DNA replication, Nucleic Acid Hybridization, DNA replication origin, Mutagenesis, Insertional, Insect Science, DNA, Viral, Minute Virus of Mice, Origin recognition complex, Chromosome Deletion, Plasmids, Research Article

Abstract

Mutations were introduced into plasmid pMM984, a full-length infectious clone of the fibrotropic strain of minute virus of mice, to identify cis-acting genetic elements required for the excision and replication of the viral genome. The replicative capacity of these mutants was measured directly, using an in vivo transient DNA replication assay following transfection of plasmids into murine A9 cells and primate COS-7 cells. Experiments with subgenomic constructs indicated that both viral termini must be present on the same DNA molecule for replication to occur and that the viral nonstructural protein NS-1 must be provided in trans. The necessary sequences were located within 1,084 and 807 nucleotides of the 3' and 5' ends of the minute virus of mice genome, respectively. The inhibitory effect of deletions within the 206-bp 5'-terminal palindrome demonstrated that these sequences comprise a cis-acting genetic element that is absolutely essential for the excision and replication of viral DNA. The results further indicated a requirement for a stem-plus-arms T structure as well as for the formation of a simple hairpin. In addition, the removal of one copy of a tandemly arranged 65-bp repeat found 94 nucleotides inboard of the 5'-terminal palindrome inhibited viral DNA replication in cis by 10- and just greater than 100-fold in A9 and COS-7 cells, respectively. The latter results define a novel genetic element within the 65-bp repeated sequence, distinct from the terminal palindrome, that is capable of regulating minute virus of mice DNA replication in a species-specific manner.

Published

1991