Your search keyword '"Petherbridge L"' showing total 20 results

1. Pre-Clinical Development of an Adenovirus Vector Based RSV and Shingles Vaccine Candidate.

Author

Petherbridge L, Davis C, Robinson A, Evans T, and Sebastian S

Abstract

Respiratory syncytial virus (RSV) infection and shingles are two viral diseases that affect older adults, and a combined vaccine to protect against both could be beneficial. RSV infection causes hospitalisations and significant morbidity in both children and adults and can be fatal in the elderly. The RSV fusion (F) envelope glycoprotein induces a strong RSV-neutralising antibody response and is the target of protective immunity in the first RSV vaccine for older adults, recently approved by the FDA. An initial childhood infection with the varicella zoster virus (VZV) results in chickenpox disease, but reactivation in older adults can cause shingles. This reactivation in sensory and autonomic neurons is characterized by a skin-blistering rash that can be accompanied by prolonged pain. The approved protein-in-adjuvant shingles vaccine induces VZV glycoprotein E (gE)-fspecific antibody and CD4 + T cell responses and is highly effective. Here we report the evaluation of RSV/shingles combination vaccine candidates based on non-replicating chimpanzee adenovirus (ChAd) vectors. We confirmed the cellular and humoral immunogenicity of the vaccine vectors in mice using T cell and antibody assays. We also carried out an RSV challenge study in cotton rats which demonstrated protective efficacy following a homologous prime-boost regimen with our preferred vaccine candidate.

Published

2023

2. Response to 'pervasive sequence patents cover the entire human genome'.

Author

Tu S, Holman C, Mossoff A, Sichelman T, Risch M, Conteras JL, Heled Y, Dolin G, and Petherbridge L

Abstract

A response to Pervasive sequence patents cover the entire human genome by J Rosenfeld and C Mason. Genome Med 2013, 5:27. See related Correspondence by Rosenfeld and Mason, http://genomemedicine.com/content/5/3/27 and related letter by Rosenfeld and Mason, http://genomemedicine.com/content/6/2/15.

Published

2014

3. Novel microRNAs encoded by duck enteritis virus.

Author

Yao Y, Smith LP, Petherbridge L, Watson M, and Nair V

Subjects

Animals, Cells, Cultured, Chickens, Fibroblasts virology, High-Throughput Nucleotide Sequencing, Mardivirus genetics, MicroRNAs genetics, RNA, Viral genetics

Abstract

Duck enteritis virus (DEV) is an important herpesvirus pathogen associated with acute, highly contagious lethal disease in waterfowls. Using a deep sequencing approach on RNA from infected chicken embryo fibroblast cultures, we identified several novel DEV-encoded micro (mi)RNAs. Unlike most mardivirus-encoded miRNAs, DEV-encoded miRNAs mapped mostly to the unique long region of the genome. The precursors of DEV miR-D18 and miR-D19 overlapped with each other, suggesting similarities to miRNA-offset RNAs, although only the DEV-miR-D18-3p was functional in reporter assays. Identification of these novel miRNAs will add to the growing list of virus-encoded miRNAs enabling the exploration of their roles in pathogenesis.

Published

2012

4. Differential quantification of cloned CVI988 vaccine strain and virulent RB-1B strain of Marek's disease viruses in chicken tissues, using real-time PCR.

Author

Baigent SJ, Smith LP, Petherbridge LJ, and Nair VK

Subjects

Animals, Chickens, Mardivirus immunology, Marek Disease immunology, Marek Disease Vaccines immunology, Poultry Diseases immunology, DNA, Viral analysis, Mardivirus genetics, Marek Disease virology, Marek Disease Vaccines genetics, Polymerase Chain Reaction veterinary, Poultry Diseases virology

Abstract

The 'gold standard' vaccine against Marek's disease in poultry is the CVI988/Rispens virus, which is not easily distinguishable, antigenically or genetically, from virulent Marek's disease herpesvirus. Accurate differential measurement of the CVI988 vaccine and virulent viruses is important to investigate mechanisms of vaccinal protection. Minimal sequence differences between CVI988 and virulent MDV strains restrict the application of molecular diagnostic methods such as real-time PCR to distinguish between these viruses. The use of bacterial-artificial-chromosome (BAC) cloned CVI988 virus, which carries the BAC vector sequences in place of the U(s)2 gene, allows its differential quantification from virulent strains using real-time PCR assays that target the BAC vector sequence and the U(S)2 gene respectively. These novel assays allowed investigation of replication of both serotype-1 vaccine virus (cloned CVI988) and challenge virus (RB-1B strain) in tissues of individual chickens in an experimental vaccination-challenge model of Marek's disease., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2011

5. Genotypic characterization of two bacterial artificial chromosome clones derived from a single DNA source of the very virulent gallid herpesvirus-2 strain C12/130.

Author

Spatz SJ, Smith LP, Baigent SJ, Petherbridge L, and Nair V

Subjects

Animals, Cells, Cultured, Chickens, DNA, Viral metabolism, Genotype, Herpesvirus 2, Gallid isolation & purification, Herpesvirus 2, Gallid pathogenicity, Herpesvirus 2, Gallid physiology, Molecular Sequence Data, Mutation, Virulence, Chromosomes, Artificial, Bacterial genetics, DNA, Viral genetics, Herpesvirus 2, Gallid genetics, Marek Disease virology

Abstract

The identification of specific genetic changes associated with differences in the pathogenicity of Marek's disease virus strains (GaHV-2) has been a formidable task due to the large number of mutations in mixed-genotype populations within DNA preparations. Very virulent UK isolate C12/130 induces extensive lymphoid atrophy, neurological manifestations and early mortality in young birds. We have recently reported the construction of several independent full-length bacterial artificial chromosome (BAC) clones of C12/130 capable of generating fully infectious viruses with significant differences in their pathogenicity profiles. Two of these clones (vC12/130-10 and vC12/130-15), which showed differences in virulence relative to each other and to the parental strain, had similar replication kinetics both in vitro and in vivo in spite of the fact that vC12/130-15 was attenuated. To investigate the possible reasons for this, the nucleotide sequences of both clones were determined. Sequence analysis of the two genomes identified mutations within eight genes. A single 494 bp insertion was identified within the genome of the virulent vC12/130-10 clone. Seven non-synonymous substitutions distinguished virulent vC12/130-10 from that of attenuated vC12/130-15. By sequencing regions of parental DNA that differed between the two BAC clones, we confirmed that C12/130 does contain these mutations in varying proportions. Since the individual reconstituted BAC clones were functionally attenuated in vivo and derived from a single DNA source of phenotypically very virulent C12/130, this suggests that the C12/130 virus population exists as a collection of mixed genotypes.

Published

2011

6. Critical role of the virus-encoded microRNA-155 ortholog in the induction of Marek's disease lymphomas.

Author

Zhao Y, Xu H, Yao Y, Smith LP, Kgosana L, Green J, Petherbridge L, Baigent SJ, and Nair V

Subjects

Animals, Base Sequence, Cells, Cultured, Chick Embryo, Chickens, Fibroblasts cytology, Fibroblasts metabolism, Genome, Viral, Herpesvirus 2, Gallid growth & development, Humans, Lymphoma pathology, Lymphoma prevention & control, Marek Disease pathology, Marek Disease prevention & control, Molecular Sequence Data, Mutation genetics, RNA, Viral genetics, Vaccination, Herpesvirus 2, Gallid genetics, Lymphoma etiology, Marek Disease etiology, MicroRNAs genetics

Abstract

Notwithstanding the well-characterised roles of a number of oncogenes in neoplastic transformation, microRNAs (miRNAs) are increasingly implicated in several human cancers. Discovery of miRNAs in several oncogenic herpesviruses such as KSHV has further highlighted the potential of virus-encoded miRNAs to contribute to their oncogenic capabilities. Nevertheless, despite the identification of several possible cancer-related genes as their targets, the direct in vivo role of virus-encoded miRNAs in neoplastic diseases such as those induced by KSHV is difficult to demonstrate in the absence of suitable models. However, excellent natural disease models of rapid-onset Marek's disease (MD) lymphomas in chickens allow examination of the oncogenic potential of virus-encoded miRNAs. Using viruses modified by reverse genetics of the infectious BAC clone of the oncogenic RB-1B strain of MDV, we show that the deletion of the six-miRNA cluster 1 from the viral genome abolished the oncogenicity of the virus. This loss of oncogenicity appeared to be primarily due to the single miRNA within the cluster, miR-M4, the ortholog of cellular miR-155, since its deletion or a 2-nucleotide mutation within its seed region was sufficient to inhibit the induction of lymphomas. The definitive role of this miR-155 ortholog in oncogenicity was further confirmed by the rescue of oncogenic phenotype by revertant viruses that expressed either the miR-M4 or the cellular homolog gga-miR-155. This is the first demonstration of the direct in vivo role of a virus-encoded miRNA in inducing tumors in a natural infection model. Furthermore, the use of viruses deleted in miRNAs as effective vaccines against virulent MDV challenge, enables the prospects of generating genetically defined attenuated vaccines.

Published

2011

7. Comparative efficacy of BAC-derived recombinant SB-1 vaccine and the parent wild type strain in preventing replication, shedding and disease induced by virulent Marek's disease virus.

Author

Singh SM, Baigent SJ, Petherbridge LJ, Smith LP, and Nair VK

Subjects

Animals, Chickens, Chromosomes, Artificial, Bacterial, Cloning, Molecular, DNA, Recombinant, DNA, Viral genetics, Marek Disease virology, Virulence, Herpesvirus 2, Gallid pathogenicity, Marek Disease prevention & control, Marek Disease Vaccines immunology, Vaccines, DNA immunology, Virus Replication physiology, Virus Shedding physiology

Abstract

A widely used vaccine against Marek's disease (MD) in poultry is the virus SB-1, which is antigenically-related to the causative agent, Marek's disease herpesvirus. We recently cloned the SB-1 genome as an infectious bacterial artificial chromosome, BAC, (pSB-1). The protective efficacies and replication kinetics of pSB-1 and the parent strain (SB-1) were compared in an experimental model of MD induced by a virulent strain, RB-1B. Although vaccine virus replication and shedding was lower for pSB-1 than for SB-1, both vaccines reduced replication and shedding of RB-1B, and were equally effective in protecting chickens against MD. With the cloning of pSB-1, we have now generated full length genomic clones of MD vaccine virus strains belonging to each of the three serotypes. Vaccine viruses derived from each of these clones demonstrated protective efficacies at levels similar to those produced by the respective parent viruses, demonstrating their suitability to be used as vaccine candidates., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

8. Functional evaluation of the role of reticuloendotheliosis virus long terminal repeat (LTR) integrated into the genome of a field strain of Marek's disease virus.

Author

Sun AJ, Xu XY, Petherbridge L, Zhao YG, Nair V, and Cui ZZ

Subjects

Animals, Birds virology, DNA, Viral chemistry, DNA, Viral genetics, Immunosuppression Therapy, Marek Disease immunology, Marek Disease transmission, Marek Disease virology, Molecular Sequence Data, Sequence Analysis, DNA, Sequence Deletion, Mardivirus genetics, Mardivirus pathogenicity, Marek Disease pathology, Mutagenesis, Insertional, Recombination, Genetic, Reticuloendotheliosis virus genetics, Terminal Repeat Sequences genetics

Abstract

MDV-GX0101 is a field strain of Marek's disease virus with a naturally occurring insertion of the reticuloendotheliosis virus (REV) LTR fragment. In order to study the biological properties of REV-LTR insertion in the MDV genome, we constructed a full-length infectious BAC clone of MDV-GX0101 strain and deleted the LTR sequences by BAC mutagenesis. The pathogenic properties of the LTR-deleted virus were evaluated in infected SPF birds. The study demonstrated that the LTR-deleted virus had a stronger inhibitory effect on the growth rates of the infected birds and induced stronger immunosuppressive effects. Surprisingly, however, the ability for horizontal transmission of the LTR-deleted virus appeared to be significantly weaker than its parental LTR-intact virus. Even though the precise molecular mechanisms are still not clear, the results of our studies demonstrate that the retention of the REV-LTR in the MDV genome decreases its pathogenic effects but increases its potential for horizontal transmission., (Copyright 2009 Elsevier Inc. All rights reserved.)

Published

2010

9. The 5' leader of the mRNA encoding the marek's disease virus serotype 1 pp14 protein contains an intronic internal ribosome entry site with allosteric properties.

Author

Tahiri-Alaoui A, Matsuda D, Xu H, Panagiotis P, Burman L, Lambeth LS, Petherbridge L, James W, Mauro V, and Nair V

Subjects

Allosteric Regulation, Animals, Cells, Cultured, Codon, Genes, RNA Caps, RNA, Messenger, 5' Untranslated Regions, Herpesvirus 2, Gallid genetics, Introns, Ribosomes metabolism, Viral Proteins genetics

Abstract

We demonstrate the presence of a functional internal ribosome entry site (IRES) within the 5' leader (designated 5L) from a variant of bicistronic mRNAs that encode the pp14 and RLORF9 proteins from Marek's disease virus (MDV) serotype 1. Transcribed as a 1.8-kb family of immediate-early genes, the mature bicistronic mRNAs have variable 5' leader sequences due to alternative splicing or promoter usage. Consequently, the presence or absence of the 5L IRES in the mRNA dictates the mode of pp14 translation and leads to the production of two pp14 isoforms that differ in their N-terminal sequences. Real-time reverse transcription-quantitative PCR indicates that the mRNA variants with the 5L IRES is two to three times more abundant in MDV-infected and transformed cells than the mRNA variants lacking the 5L IRES. A common feature to all members of the 1.8-kb family of transcripts is the presence of an intercistronic IRES that we have previously shown to control the translation of the second open reading frame (i.e., RLORF9). Investigation of the two IRESs residing in the same bicistronic reporter mRNA revealed functional synergism for translation efficiency. In analogy with allosteric models in proteins, we propose IRES allostery to describe such a novel phenomenon. The functional implications of our findings are discussed in relation to host-virus interactions and translational control.

Published

2009

10. Interaction of Marek's disease virus oncoprotein Meq with heat-shock protein 70 in lymphoid tumour cells.

Author

Zhao Y, Kurian D, Xu H, Petherbridge L, Smith LP, Hunt L, and Nair V

Subjects

Amino Acid Sequence, Animals, Chick Embryo, Disease Models, Animal, HSP70 Heat-Shock Proteins genetics, Herpesvirus 2, Gallid chemistry, Herpesvirus 2, Gallid genetics, Lymphoma virology, Marek Disease virology, Molecular Sequence Data, Oncogene Proteins, Viral chemistry, Oncogene Proteins, Viral genetics, Protein Binding, Specific Pathogen-Free Organisms, HSP70 Heat-Shock Proteins metabolism, Herpesvirus 2, Gallid metabolism, Lymphoma metabolism, Marek Disease metabolism, Oncogene Proteins, Viral metabolism

Abstract

Marek's disease virus (MDV) is a highly oncogenic alphaherpesvirus that induces the rapid onset of T-cell lymphomas in poultry. The MDV-encoded oncoprotein Meq plays an important role in oncogenicity, as its deletion abolishes the ability of the virus to induce tumours. It has been shown previously that Meq oncogenicity is linked to its interaction with C-terminal binding protein 1 (CtBP), a property also shared by other virus-encoded oncoproteins such as adenovirus E1A and Epstein-Barr virus EBNA3A and -3C. Therefore, this study examined whether Meq also shares the properties of these viral oncoproteins in interacting with other binding partners such as heat-shock protein 70 (Hsp70), a molecular chaperone protein linked to multiple cellular functions including neoplastic transformation. Confocal microscopic analysis demonstrated that MDV infection induced nuclear accumulation of Hsp70 and its co-localization with Meq. Biochemical evidence of Meq-Hsp70 interaction was obtained by two-way immunoprecipitation with Meq- and Hsp70-specific antibodies. To demonstrate further the Meq-Hsp70 interaction in virus-induced lymphomas, recombinant MDV was generated expressing an N-terminal tandem affinity purification (TAP) tag-fused Meq by mutagenesis of the infectious BAC clone of the oncogenic MDV strain RB-1B. Demonstration of Hsp70 in the TAP-tag affinity purified Meq from tumours induced by the recombinant virus, using quadrupole time-of-flight tandem mass spectrometry analysis, further confirmed the Meq-Hsp70 interaction in the transformed lymphocytes. Given the well-documented evidence of the tumorigenic properties of Hsp70 and its interaction with a number of other known viral oncoproteins, demonstration of the interaction of Meq and Hsp70 is significant in MDV oncogenesis.

Published

2009

11. Cloning of Gallid herpesvirus 3 (Marek's disease virus serotype-2) genome as infectious bacterial artificial chromosomes for analysis of viral gene functions.

Author

Petherbridge L, Xu H, Zhao Y, Smith LP, Simpson J, Baigent S, and Nair V

Subjects

Animals, Chick Embryo, Gene Deletion, Genetic Vectors, Herpesvirus 3, Gallid genetics, Recombination, Genetic, Viral Proteins genetics, Chromosomes, Artificial, Bacterial genetics, Cloning, Molecular, Genome, Viral, Herpesvirus 3, Gallid physiology, Marek Disease virology, Viral Proteins physiology, Virus Replication

Abstract

Marek's disease virus serotype 2 (Gallid herpesvirus 3) is a non-pathogenic alphaherpesvirus belonging to the Mardivirus genus, used widely in live vaccines against Marek's disease. Although the complete genome sequence of the MDV-2 strain HPRS-24 has been published, very little is known about the gene functions. As a first step for carrying out functional genomic analysis of MDV-2, the full-length genome of the MDV-2 vaccine strain SB-1 was cloned as an infectious bacterial artificial chromosome (BAC) clone pSB-1. Virus reconstituted from the pSB-1 clone showed morphological and growth characteristics in cell culture very similar to the parent virus. Generation of SB-1 constructs deleted in glycoprotein E and viruses expressing Citrine-UL35 fusion protein by the application of different BAC mutagenesis techniques demonstrated the amenability of the pSB-1 clone for reverse genetics approaches to identify molecular determinants associated with different biological features of this virus. The generation of replication-competent infectious clones of SB-1, together with those of CVI988 and herpesvirus of turkey strains described previously, completes the portfolio of generating infectious BAC clones of the MD vaccine strains belonging to all the three serotypes, paving the way for the application of reverse genetics for functional analysis of immunogenic determinants of these vaccines as well as for developing novel recombinant vectors.

Published

2009

12. Self-excision of the BAC sequences from the recombinant Marek's disease virus genome increases replication and pathogenicity.

Author

Zhao Y, Petherbridge L, Smith LP, Baigent S, and Nair V

Subjects

Animals, Cells, Cultured, Chick Embryo, F Factor genetics, Herpesvirus 2, Gallid pathogenicity, Mutation, Virulence, Virus Replication, Chromosomes, Artificial, Bacterial genetics, Herpesvirus 2, Gallid physiology, Marek Disease virology

Abstract

Cloning of full length genomes of herpesviruses as bacterial artificial chromosomes (BAC) has greatly facilitated the manipulation of the genomes of several herpesviruses to identify the pathogenic determinants. We have previously reported the construction of the BAC clone (pRB-1B5) of the highly oncogenic Marek's disease virus (MDV) strain RB-1B, which has proven to be a valuable resource for elucidating several oncogenic determinants. Despite the retention of the BAC replicon within the genome, the reconstituted virus was able to induce tumours in susceptible chickens. Nevertheless, it was unclear whether the presence of the BAC influenced the full oncogenic potential of the reconstituted virus. To maximize the closeness of BAC-derived virus to the parental RB-1B strain, we modified the existing pRB-1B5 clone by restoring the Us2 and by introducing SV40-cre cassette within the loxP sites of the mini-F plasmid, to allow self-excision of the plasmid sequences in chicken cells. The reconstituted virus from the modified clone showed significant improvement in replication in vitro and in vivo. Excision of the BAC sequences also enhanced the pathogenicity to levels similar to that of the parental virus, as the cumulative incidence of Marek's disease in groups infected with the recombinant and the parental viruses showed no significant differences. Thus, we have been able to make significant improvements to the existing BAC clone of this highly oncogenic virus which would certainly increase its usefulness as a valuable tool for studies on identifying the oncogenic determinants of this major avian pathogen.

Published

2008

13. Comparative sequence analysis of a highly oncogenic but horizontal spread-defective clone of Marek's disease virus.

Author

Spatz SJ, Zhao Y, Petherbridge L, Smith LP, Baigent SJ, and Nair V

Subjects

Animals, Base Sequence, Chickens, DNA, Viral chemistry, Frameshift Mutation, Molecular Sequence Data, Phylogeny, Sequence Alignment, Sequence Analysis, DNA, Sequence Homology, Viral Proteins genetics, DNA, Viral genetics, Herpesvirus 2, Gallid genetics, Herpesvirus 2, Gallid pathogenicity, Marek Disease transmission, Marek Disease virology

Abstract

Marek's disease virus (MDV) is a cell-associated alphaherpesvirus that induces rapid-onset T-cell lymphomas in poultry. MDV isolates vary greatly in pathogenicity. While some of the strains such as CVI988 are non-pathogenic and are used as vaccines, others such as RB-1B are highly oncogenic. Molecular determinants associated with differences in pathogenicity are not completely understood. Comparison of the genome sequences of phenotypically different strains could help to identify molecular determinants of pathogenicity. We have previously reported the construction of bacterial artificial chromosome (BAC) clones of RB-1B from which fully infectious viruses could be reconstituted upon DNA transfection into chicken cells. MDV reconstituted from one of these clones (pRB-1B-5) showed similar in vitro and in vivo replication kinetics and oncogenicity as the parental virus. However, unlike the parental RB-1B virus, the BAC-derived virus showed inability to spread between birds. In order to identify the unique determinants for oncogenicity and the ''non-spreading phenotype'' of MDV derived from this clone, we determined the full-length sequence of pRB-1B-5. Comparative sequence analysis with the published sequences of strains such as Md5, Md11, and CVI988 identified frameshift mutations in RLORF1, protein kinase (UL13), and glycoproteins C (UL44) and D (US6). Comparison of the sequences of these genes with the parental virus indicated that the RLORF1, UL44, and US6 mutations were also present in the parental RB-1B stock of the virus. However with regard to UL13 mutation, the parental RB-1B stock appeared to be a mixture of wild type and mutant viruses, indicating that the BAC cloning has selected a mutant clone. Although further studies are needed to evaluate the role of these genes in the horizontal-spreading defective phenotype, our data clearly indicate that mutations in these genes do not affect the oncogenicity of MDV.

Published

2007

14. Comparative full-length sequence analysis of oncogenic and vaccine (Rispens) strains of Marek's disease virus.

Author

Spatz SJ, Petherbridge L, Zhao Y, and Nair V

Subjects

Amino Acid Sequence, Amino Acid Substitution, Base Sequence, Codon, Nonsense, DNA, Viral chemistry, Gene Order, Genes, Viral, Molecular Sequence Data, Mutation, Open Reading Frames, Phylogeny, Recombination, Genetic, Repetitive Sequences, Nucleic Acid, Selection, Genetic, Sequence Alignment, Sequence Analysis, DNA, Viral Proteins chemistry, Viral Proteins genetics, DNA, Viral genetics, Genome, Viral, Mardivirus genetics, Viral Vaccines genetics

Abstract

The complete DNA sequence of the Marek's disease virus serotype 1 vaccine strain CVI988 was determined and consists of 178 311 bp with an overall gene organization identical to that of the oncogenic strains. In examining open reading frames (ORFs), nine differ between vaccine and oncogenic strains. A 177 bp insertion was identified in the overlapping genes encoding the Meq, RLORF6 and 23 kDa proteins of CVI988. Three ORFs are predicted to encode truncated proteins. One, designated 49.1, overlaps the gene encoding the large tegument protein UL36 and encodes a severely truncated protein of 34 aa. The others, ORF5.5/ORF75.91 and ORF3.0/78.0, located in the repeat regions (diploid), encode a previously unidentified ORF of 52 aa and a truncated version of the virus-encoded chemokine (vIL-8), respectively. Subtle genetic changes were identified in the two ORFs encoding tegument proteins UL36 and UL49. Only one diploid ORF (ORF6.2/ORF75.6) present in the genomes of the three virulent strains is absent in the CVI988-BAC genome. Seventy non-synonymous amino acid substitutions were identified that could differentiate CVI988-BAC from all three oncogenic strains collectively. Estimates of the non-synonymous to synonymous substitution ratio (omega) indicate that CVI988 ORFs are generally under purifying selection (omega<1), whereas UL39, UL49, UL50, RLORF6 and RLORF7 (Meq) appear to evolve under relaxed selective constraints. No CVI988 ORF was found to be under positive evolutionary selection (omega>>1).

Published

2007

15. Oncogenicity of virulent Marek's disease virus cloned as bacterial artificial chromosomes.

Author

Petherbridge L, Brown AC, Baigent SJ, Howes K, Sacco MA, Osterrieder N, and Nair VK

Subjects

Animals, Chick Embryo, Gene Dosage, Mardivirus genetics, Mardivirus physiology, Marek Disease etiology, Virulence, Virus Replication, Chromosomes, Artificial, Bacterial, Mardivirus pathogenicity

Abstract

Marek's disease virus (MDV) is an oncogenic alphaherpesvirus that induces T-cell lymphomas in poultry. We report the construction of bacterial artificial chromosome (BAC) clones of the highly oncogenic RB-1B strain by inserting mini-F vector sequences into the U(S)2 locus. MDV reconstituted from two BAC clones induced rapid-onset lymphomas similar to those induced by the wild-type virus. Virus reconstituted from another BAC clone that showed a 7.7-kbp deletion in the internal and terminal unique long repeat regions was nononcogenic, suggesting that the deleted region may be associated with oncogenicity. The generation of the oncogenic BAC clones of MDV is a significant step in unraveling the oncogenic determinants of this virus.

Published

2004

16. Replication-competent bacterial artificial chromosomes of Marek's disease virus: novel tools for generation of molecularly defined herpesvirus vaccines.

Author

Petherbridge L, Howes K, Baigent SJ, Sacco MA, Evans S, Osterrieder N, and Nair V

Subjects

Amino Acid Sequence, Base Sequence, DNA Primers, Mardivirus physiology, Molecular Sequence Data, Oncogene Proteins, Viral genetics, Sequence Homology, Nucleic Acid, Chromosomes, Artificial, Bacterial, Herpesviridae immunology, Mardivirus genetics, Vaccines, DNA genetics, Viral Vaccines genetics, Virus Replication genetics

Abstract

Marek's disease (MD), a highly infectious disease caused by an oncogenic herpesvirus, is one of the few herpesvirus diseases against which live attenuated vaccines are used as the main strategy for control. We have constructed bacterial artificial chromosomes (BACs) of the CVI988 (Rispens) strain of the virus, the most widely used and effective vaccine against MD. Viruses derived from the BAC clones were stable after in vitro and in vivo passages and showed characteristics and growth kinetics similar to those of the parental virus. Molecular analysis of the individual BAC clones showed differences in the structure of the meq gene, indicating that the commercial vaccine contains virus populations with distinct genomic structures. We also demonstrate that, contrary to the published data, the sequence of the L-meq of the BAC clone did not show any frameshift. Virus stocks derived from one of the BAC clones (clone 10) induced 100 percent protection against infection by the virulent strain RB1B, indicating that BAC-derived viruses could be used with efficacies similar to those of the parental CVI988 vaccines. As a DNA vaccine, this BAC clone was also able to induce protection in 6 of 20 birds. Isolation of CVI988 virus from all of these six birds suggested that immunity against challenge was probably dependent on the reconstitution of the virus in vivo and that such viruses are also as immunogenic as the in vitro-grown BAC-derived or parental vaccine viruses. Although the reasons for the induction of protection only in a proportion of birds (33.3%) that received the DNA vaccine are not clear, this is most likely to be related to the suboptimal method of DNA delivery. The construction of the CVI988 BAC is a major step towards understanding the superior immunogenic features of CVI988 and provides the opportunity to exploit the power of BAC technology for generation of novel molecularly defined vaccines.

Published

2003

17. The viral envelope is a major determinant for the induction of lymphoid and myeloid tumours by avian leukosis virus subgroups A and J, respectively.

Author

Chesters PM, Howes K, Petherbridge L, Evans S, Payne LN, and Venugopal K

Subjects

Alpharetrovirus genetics, Animals, Avian Leukosis Virus genetics, Avian Myeloblastosis Virus genetics, Base Sequence, Cell Lineage, Chick Embryo, DNA, Viral, Gene Rearrangement, Genes, myc, Lymphocytes, Molecular Sequence Data, Myeloid Cells, Recombination, Genetic, Viral Envelope Proteins genetics, Virus Integration, Alpharetrovirus physiology, Avian Leukosis virology, Avian Leukosis Virus physiology, Avian Myeloblastosis Virus physiology, Leukemia, Lymphoid virology, Leukemia, Myeloid virology, Viral Envelope Proteins physiology

Abstract

Among the six envelope subgroups of avian leukosis virus (ALV) that infect chickens, subgroups A (ALV-A) and J (ALV-J) are the most pathogenic and widespread among commercial chicken populations. While ALV-A is predominantly associated with lymphoid leukosis (LL) and less frequently with erythroblastosis (EB), ALV-J mainly induces tumours of the myeloid lineage. In order to examine the basis for the lineage specificity of tumour induction by these two ALV subgroups, we constructed two chimeric viruses by substituting the env genes into the reciprocal proviral clones. The chimeric HPRS-103(A) virus carrying the subgroup A env gene is identical to ALV-J prototype virus HPRS-103 except for the env gene, and the chimeric RCAS(J) virus carrying the subgroup J env gene is identical to the parent replication-competent ALV-A vector RCAS except for the env gene. In experimentally inoculated chickens, HPRS-103(A) virus induced LL and EB similar to ALV-A isolates such as RAV-1, while RCAS(J) virus induced myeloid leukosis (ML) and EB, similar to ALV-J, suggesting that the env gene is the major determinant for the lineage-specific oncogenicity. There were genetic differences in susceptibility to tumour induction between line 0 and line 15(I) chickens, indicating that in addition to the env gene, other viral or host factors could also serve as determinants for oncogenicity. Induction of both LL and ML by the two chimeric viruses occurred through the activation of c-myc, while the EB tumours were induced by activation of the c-erbB oncogene.

Published

2002

18. Expression of MK6a dominant-negative and C-terminal mutant transgenes in mice has distinct phenotypic consequences in the epidermis and hair follicle.

Author

Wojcik SM, Imakado S, Seki T, Longley MA, Petherbridge L, Bundman DS, Bickenbach JR, Rothnagel JA, and Roop DR

Subjects

Age of Onset, Alopecia genetics, Amino Acid Sequence, Animals, Animals, Newborn, Epidermis pathology, Epidermis ultrastructure, Gene Expression, Hair Follicle pathology, Hair Follicle ultrastructure, Keratins biosynthesis, Keratins ultrastructure, Mice, Mice, Inbred BALB C, Mice, Transgenic, Microscopy, Electron, Molecular Sequence Data, Mutagenesis, Site-Directed, Phenotype, Protein Isoforms biosynthesis, Protein Isoforms genetics, Skin Diseases genetics, Skin Diseases pathology, Time Factors, Epidermis metabolism, Genes, Dominant, Hair Follicle metabolism, Keratins genetics, Transgenes

Abstract

Mouse keratin 6a (MK6a) is constitutively expressed in a single cell layer of the outer root sheath (ORS) of hair follicles, but its synthesis can be induced in interfollicular epidermis including the basal cell layer in response to perturbing stimuli. A basally inducible human K6 (HK6) isoform has not been described, and it is not clear which of the known HK6 isoforms is expressed in the ORS. In this study we show that expression of a dominant-negative MK6a construct (Delta2B-P) in the interfollicular epidermis caused severe blistering and neonatal lethality, suggesting that mutations in a yet to be identified basally expressed HK6 isoform might result in a severe blistering phenotype. Surviving Delta2B-P animals showed transgene expression only in isolated epidermal cells and not in all cells of the ORS, but nevertheless developed severe alopecia. Expression of two different C-terminal mutant transgenes also caused alopecia while a third C-terminal mutant had no phenotypic conse- quences. Electron microscopy revealed that Delta2B-P expression resulted in the collapse of keratin filaments, while destruction of hair follicles in the two phenotypic C-terminal mutant lines occurred in the absence of filament abnormalities. The latter finding indicates that the innermost ORS cells are uniquely sensitive to expression of even slightly altered K6 proteins, suggesting that mutations affecting an HK6 isoform expressed in this cell layer could result in alopecia in humans as well.

Published

1999

19. Differences in both inositol 1,4,5-trisphosphate mass and inositol 1,4,5-trisphosphate receptors between normal and dystrophic skeletal muscle cell lines.

Author

Liberona JL, Powell JA, Shenoi S, Petherbridge L, Caviedes R, and Jaimovich E

Subjects

Actinin analysis, Animals, Calcium Channels metabolism, Cell Fractionation, Cell Line, Dystrophin deficiency, Dystrophin genetics, Electrophysiology, Humans, Inositol 1,4,5-Trisphosphate metabolism, Inositol 1,4,5-Trisphosphate pharmacology, Inositol 1,4,5-Trisphosphate Receptors, Membrane Potentials drug effects, Membrane Potentials physiology, Mice, Mice, Inbred C57BL, Mice, Inbred mdx, Muscle, Skeletal chemistry, Muscle, Skeletal cytology, Potassium Chloride pharmacology, Radioligand Assay, Receptors, Cytoplasmic and Nuclear agonists, Receptors, Cytoplasmic and Nuclear metabolism, Ryanodine pharmacology, Tritium, Calcium Channels analysis, Inositol 1,4,5-Trisphosphate analysis, Muscle, Skeletal metabolism, Muscular Dystrophy, Animal metabolism, Receptors, Cytoplasmic and Nuclear analysis

Abstract

Human normal (RCMH) and Duchenne muscular dystrophy (RCDMD) cell lines, as well as newly developed normal and dystrophic murine cell lines, were used for the study of both changes in inositol 1,4,5-trisphosphate (IP3) mass and IP3 binding to receptors. Basal levels of IP3 were increased two- to threefold in dystrophic human and murine cell lines compared to normal cell lines. Potassium depolarization induced a time-dependent IP3 rise in normal human cells and cells of the myogenic mouse cell line (129CB3), which returned to their basal levels after 60 s. However, in the human dystrophic cell line (RCDMD), IP3 levels remained high up to 200 s after potassium depolarization. Expression of IP3 receptors was studied measuring specific binding of 3H-IP3 in the murine cell lines (normal 129CB3 and dystrophic mdx XLT 4-2). All the cell lines bind 3H-IP3 with relatively high affinity (Kd: between 40 and 100 nmol/L). IP3 receptors are concentrated in the nuclear fraction, and their density is significantly higher in dystrophic cells compared to normal. These findings together with high basal levels of IP3 mass suggest a possible role for this system in the deficiency of intracellular calcium regulation in Duchenne muscular dystrophy.

Published

1998

20. Formation of triads without the dihydropyridine receptor alpha subunits in cell lines from dysgenic skeletal muscle.

Author

Powell JA, Petherbridge L, and Flucher BE

Subjects

Animals, Calcium Channels genetics, Calcium Channels, L-Type, Cell Line, Membrane Fusion, Muscle Proteins genetics, Muscle, Skeletal cytology, Muscle, Skeletal ultrastructure, Rats, Ryanodine Receptor Calcium Release Channel, Calcium Channels metabolism, Muscle Proteins metabolism, Muscle, Skeletal metabolism

Abstract

Muscular dysgenesis (mdg/mdg), a mutation of the skeletal muscle dihydropyridine receptor (DHPR) alpha 1 subunit, has served as a model to study the functions of the DHPR in excitation-contraction coupling and its role in triad formation. We have investigated the question of whether the lack of the DHPR in dysgenic skeletal muscle results in a failure of triad formation, using cell lines (GLT and NLT) derived from dysgenic (mdg/mdg) and normal (+/+) muscle, respectively. The lines were generated by transfection of myoblasts with a plasmid encoding a Large T antigen. Both cell lines express muscle-specific proteins and begin organization of sarcomeres as demonstrated by immunocytochemistry. Similar to primary cultures, dysgenic (GLT) myoblasts show a higher incidence of cell fusion than their normal counterparts (NLT). NLT myotubes develop spontaneous contractile activity, and fluorescent Ca2+ recordings show Ca2+ release in response to depolarization. In contrast, GLTs show neither spontaneous nor depolarization-induced Ca2+ transients, but do release Ca2+ from the sarcoplasmic reticulum (SR) in response to caffeine. Despite normal transverse tubule (T-tubule) formation, GLT myotubes lack the alpha 1 subunit of the skeletal muscle DHPR, and the alpha 2 subunit is mistargeted. Nevertheless, the ryanodine receptor (RyR) frequently develops its normal, clustered organization in the absence of both DHPR alpha subunits in the T-tubules. In EM, these RyR clusters correspond to T-tubule/SR junctions with regularly spaced feet. These findings provide conclusive evidence that interactions between the DHPR and RyR are not involved in the formation of triad junctions or in the normal organization of the RyR in the junctional SR.

Published

1996