Your search keyword '"Stanley MA"' showing total 7 results

1. Cell-mediated immune responses to COPV early proteins.

Author

Jain S, Moore RA, Anderson DM, Gough GW, and Stanley MA

Subjects

Animals, Disease Models, Animal, Dog Diseases immunology, Dog Diseases virology, Dogs, Female, Lambdapapillomavirus metabolism, Lambdapapillomavirus pathogenicity, Male, Mouth Mucosa immunology, Mouth Neoplasms immunology, Mouth Neoplasms prevention & control, Mouth Neoplasms virology, Papillomavirus Infections immunology, Papillomavirus Infections prevention & control, Vaccination, Vaccines, DNA administration & dosage, Viral Vaccines administration & dosage, Dog Diseases prevention & control, Lambdapapillomavirus immunology, Papillomavirus Infections veterinary, T-Lymphocytes immunology, Vaccines, DNA immunology, Viral Proteins immunology, Viral Vaccines immunology

Abstract

Cell-mediated immunity plays a key role in the regression of papillomavirus-induced warts and intra-epithelial lesions but the target antigens that induce this response are not clear. Canine oral papillomavirus (COPV) infection of the oral cavity in dogs is a well-characterized model of mucosal papillomavirus infection that permits analysis of the immune events during the infectious cycle. In this study we show that during the COPV infectious cycle, systemic T cell responses to peptides of several early proteins particularly the E2 protein, as assayed by delayed type hypersensitivity, lymphoproliferation and IFN-gamma ELISPOT, can be detected. The maximal response occurs in a narrow time window that coincides with maximal viral DNA replication and wart regression: thereafter, systemic T cell responses to early proteins decline quite rapidly. Vaccination using particle-mediated immunotherapeutic delivery (PMID) of codon-modified COPV E2 and E1 genes induces strong antigen-specific cell-mediated immune responses in the vaccinated animals. These data show that therapeutic immunization by PMID with codon-modified E2 is completely effective, that to E1 is partially protective, that this correlates with the intensity of antigen-specific cell-mediated immune responses and, further, they emphasize the importance of these responses and the route of immunization in the generation of protective immunity.

Published

2006

2. Protection of beagle dogs from mucosal challenge with canine oral papillomavirus by immunization with recombinant adenoviruses expressing codon-optimized early genes.

Author

Johnston KB, Monteiro JM, Schultz LD, Chen L, Wang F, Ausensi VA, Dell EC, Santos EB, Moore RA, Palker TJ, Stanley MA, and Jansen KU

Subjects

Animals, Cells, Cultured, Dogs, Enzyme-Linked Immunosorbent Assay, Female, Injections, Subcutaneous, Interferon-gamma analysis, Leukocytes, Mononuclear immunology, Mouth Neoplasms immunology, Neoplasms, Experimental immunology, Oncogene Proteins, Viral genetics, Oncogene Proteins, Viral immunology, Papillomavirus Infections immunology, Recombination, Genetic, Adenoviridae genetics, Codon, Genetic Vectors administration & dosage, Mouth Neoplasms prevention & control, Neoplasms, Experimental prevention & control, Papillomaviridae genetics, Papillomavirus Infections prevention & control, Vaccination, Vaccines, DNA administration & dosage

Abstract

Replication-deficient adenoviral (rAd5) vaccines containing codon-optimized E1, E2, E4, and E7 genes of canine oral papillomavirus (COPV) were tested singly or in combination to determine which vaccines could protect against mucosal challenge with COPV. In three studies, groups of 4-6 beagle dogs were immunized subcutaneously (s.c.) with 10(11) rAd5 at 8-10 weeks and 4-6 weeks prior to challenge with infectious COPV particles at multiple oral mucosal sites. Control dogs were immunized with equivalent doses of rAd5 expressing human papillomavirus (HPV) type 16 L1 (rAd5-HPV-16 L1). In the first study, complete protection from COPV-induced papillomas was achieved by immunization with rAd5 vaccine combinations expressing either E1 + E2 or E1 + E2 + E4 + E7; whereas two of six dogs immunized with rAd5-E4 + rAd5-E7 and six of six rAd5-HPV16-L1-immunized control dogs developed oral papillomas. In two subsequent studies, rAd5-E1 and rAd5-E2 vaccines were tested singly or in combination to assess levels of protective immunity to COPV challenge. Subcutaneous immunization with either one or two doses of rAd5 expressing the COPV E1 and E2 genes could protect > 90% of challenged dogs from wart formation. In contrast, all eight dogs immunized with rAd5-HPV-16 L1 developed papillomas at multiple sites. Protection was accompanied by significant IFN-gamma responses to COPV E1 and E2 peptides. Partial protection was conferred by two immunizations with either rAd5-E1 (6 of 9 protected) or rAd5-E2 (8 of 9 protected). These data indicate that rAd5 expressing papillomavirus E1 and E2 proteins can induce strong protective responses even in outbred populations under practical immunization conditions.

Published

2005

3. Therapeutic immunisation with COPV early genes by epithelial DNA delivery.

Author

Moore RA, Walcott S, White KL, Anderson DM, Jain S, Lloyd A, Topley P, Thomsen L, Gough GW, and Stanley MA

Subjects

Animals, Capsid Proteins administration & dosage, Capsid Proteins genetics, Capsid Proteins immunology, Cell Line, Disease Models, Animal, Dogs, Humans, Immunization, Mouth Mucosa virology, Papilloma virology, Papillomaviridae genetics, Papillomavirus Infections drug therapy, Papillomavirus Infections virology, Plasmids, Vaccines, DNA administration & dosage, Vaccines, DNA immunology, Viral Proteins administration & dosage, Viral Proteins genetics, Viral Vaccines administration & dosage, Viral Vaccines immunology, Epithelium virology, Papilloma drug therapy, Papillomaviridae immunology, Vaccines, DNA therapeutic use, Viral Proteins immunology, Viral Vaccines therapeutic use

Abstract

Following challenge with COPV (canine oral papillomavirus), DNA plasmids encoding COPV L1, E1 or E2 protein were delivered into oral mucosal and cutaneous sites in beagles using particle-mediated immunotherapeutic delivery (PMID). Two weeks post-challenge, a priming dose of 8 microg DNA was delivered followed by a booster dose after a further two weeks. A group of control dogs were vaccinated using plasmid DNA encoding Hepatitis B virus surface (HBVs) gene. All of the control animals developed warts at the vast majority of sites (94%). All of the animals given wild type L1, E1, or E2 developed warts at most sites (88%, 75%, and 88%, respectively). The animals given codon optimised E2 however, were protected from wart growth with only one tiny lesion seen on a single animal that persisted for only a few days. The E1 codon optimised group was also significantly protected with a far lower number of smaller warts (48%) that persisted for a shorter duration. These data suggest that therapeutic immunisation by PMID with papillomavirus early genes is effective and emphasizes the importance of antigen load in the generation of protective responses to papillomavirus proteins.

Published

2003

4. Intraepithelial DNA immunisation with a plasmid encoding a codon optimised COPV E1 gene sequence, but not the wild-type gene sequence completely protects against mucosal challenge with infectious COPV in beagles.

Author

Moore RA, Santos EB, Nicholls PK, White KL, Anderson DM, Lloyd A, Topley P, Romanos M, Thomsen L, Parmar V, Walcott S, Gough GW, and Stanley MA

Subjects

Animals, Codon, Dogs, Immunization, Mouth Mucosa virology, Mouth Neoplasms prevention & control, Papilloma prevention & control, Papillomavirus Infections prevention & control, Plasmids, Dog Diseases prevention & control, Mouth Neoplasms veterinary, Papilloma veterinary, Papillomaviridae immunology, Papillomavirus Infections veterinary, Vaccines, DNA immunology, Viral Nonstructural Proteins genetics, Viral Nonstructural Proteins immunology, Viral Vaccines immunology

Abstract

DNA plasmids encoding the open reading frames of canine oral papillomavirus (COPV) nonstructural early genes E1, E2, or E7 protein were delivered into both oral mucosal and cutaneous epithelial sites in beagle dogs using particle-mediated immunotherapeutic delivery (PMID) technology. Control dogs were vaccinated with plasmid encoding either hepatitis B virus surface antigen (HBVs) or COPV L1. Using a prophylactic immunisation protocol, a priming dose of plasmid DNA was followed by a booster dose 6 weeks later. Four weeks after boost, all dogs were challenged with infectious COPV particles. Following viral challenge, as shown previously (M. A. Stanley et al., 2001, Vaccine 19, 2783-2792), mucosal papillomas developed in the negative-control HBVs vaccinated dogs, but all animals in the COPV L1 group were fully protected from disease development. In the early gene-vaccinated groups five of six in the E1-vaccinated dogs, two of six in E2-vaccinated dogs, and three of six in the E7-vaccinated beagles developed oral papillomas. Compared to the HBVs negative-control group the oral papillomas that did develop in the early-gene vaccinated beagles were significantly smaller, shorter in duration, and fewer in number. Taken together the disease burden was markedly reduced and this was statistically significant. In a second experiment one group of animals was vaccinated with plasmid encoding the wild-type COPV E1 gene, and a separate group was vaccinated with plasmid encoding a synthetic codon-optimised COPV E1 gene sequence. None of the codon-optimised E1-vaccinated animals developed papillomas at any challenge site. However, all animals vaccinated with wild-type E1 had papillomas. These data suggest that immunisation by PMID with papillomavirus early genes can significantly impact upon subsequent disease development and that full protection can be achieved using improved vectors encoding codon-optimised gene sequences perhaps emphasizing the importance of antigen load in the generation of protective responses to papillomavirus proteins., (Copyright 2002 Elsevier Science (USA))

Published

2002

5. Detection of viral DNA and E4 protein in basal keratinocytes of experimental canine oral papillomavirus lesions.

Author

Nicholls PK, Doorbar J, Moore RA, Peh W, Anderson DM, and Stanley MA

Subjects

Animals, Capsid biosynthesis, DNA Replication, DNA, Viral biosynthesis, DNA, Viral chemistry, Disease Models, Animal, Dogs, Female, In Situ Hybridization, Mitotic Index, Mouth Mucosa virology, Oncogene Proteins, Fusion genetics, Open Reading Frames, Papillomaviridae genetics, Papillomaviridae physiology, RNA Probes, RNA, Viral chemistry, Virus Latency, Capsid Proteins, DNA, Viral isolation & purification, Keratinocytes virology, Mouth Diseases virology, Oncogene Proteins, Fusion isolation & purification, Papillomaviridae classification, Papillomavirus Infections virology, Tumor Virus Infections virology, Viral Proteins

Abstract

We studied experimental canine oral papillomavirus (COPV) infection by in situ hybridization and immunohistochemistry of weekly biopsies. After 4 weeks, viral DNA in rete ridges suggested a keratinocyte stem cell target. Abundant viral DNA was seen in E4-positive cells only. E4 was predominantly cytoplasmic but also nuclear, being concentrated in the nucleoli during wart formation. Infected cells spread laterally along the basal layer and into the parabasal layers, accompanied by E7 transcription and increased mitoses. Most of the lower epithelium was positive for viral DNA, but, in mature warts, higher levels of E4 expression and genome amplification occurred in only sporadic superficial cells. L1 expression was late and in only a subset of E4-positive cells. During regression, viral DNA was less abundant in deep epithelial layers, suggesting downregulation of replication prior to replacement of infected cells from beneath. Detection of viral DNA in post-regression tissue indicated latent infection., (Copyright 2001 Academic Press.)

Published

2001

6. Regression of canine oral papillomas is associated with infiltration of CD4+ and CD8+ lymphocytes.

Author

Nicholls PK, Moore PF, Anderson DM, Moore RA, Parry NR, Gough GW, and Stanley MA

Subjects

Animals, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes, Disease Models, Animal, Dog Diseases immunology, Dogs, Enzyme-Linked Immunosorbent Assay, Female, Humans, Immunohistochemistry, Mouth Mucosa immunology, Mouth Neoplasms immunology, Papilloma immunology, Papillomavirus Infections immunology, Remission, Spontaneous, Tumor Virus Infections immunology, Dog Diseases virology, Mouth Neoplasms veterinary, Papilloma veterinary, Papillomaviridae immunology, Papillomavirus Infections veterinary, Tumor Virus Infections veterinary

Abstract

Canine oral papillomavirus (COPV) infection is used in vaccine development against mucosal papillomaviruses. The predictable, spontaneous regression of the papillomas makes this an attractive system for analysis of cellular immunity. Immunohistochemical analysis of the timing and phenotype of immune cell infiltration revealed a marked influx of leukocytes during wart regression, including abundant CD4+ and CD8+ cells, with CD4+ cells being most numerous. Comparison of these findings, and those of immunohistochemistry using TCRalphabeta-, TCRgammadelta-, CD1a-, CD1c-, CD11a-, CD11b-, CD11c-, CD18-, CD21-, and CD49d-specific monoclonal antibodies, with previously published work in the human, ox, and rabbit models revealed important differences between these systems. Unlike bovine papillomavirus lesions, those of COPV do not have a significant gamma/delta T-cell infiltrate. Furthermore, COPV lesions had numerous CD4+ cells, unlike cottontail rabbit papillomavirus lesions. The lymphocyte infiltrate in the dog resembled that in human papillomavirus lesions, indicating that COPV is an appropriate model for human papillomavirus immunity., (Copyright 2001 Academic Press.)

Published

2001

7. Naturally occurring, nonregressing canine oral papillomavirus infection: host immunity, virus characterization, and experimental infection.

Author

Nicholls PK, Klaunberg BA, Moore RA, Santos EB, Parry NR, Gough GW, and Stanley MA

Subjects

Animals, Capsid immunology, Dog Diseases pathology, Dog Diseases virology, Dogs, Female, Mouth Neoplasms immunology, Mouth Neoplasms pathology, Mouth Neoplasms virology, Papilloma immunology, Papilloma virology, Papillomaviridae genetics, Papillomaviridae ultrastructure, Papillomavirus Infections immunology, Papillomavirus Infections pathology, Papillomavirus Infections virology, Tumor Virus Infections immunology, Tumor Virus Infections pathology, Tumor Virus Infections virology, Viral Vaccines immunology, Warts immunology, Warts virology, Capsid Proteins, Dog Diseases immunology, Mouth Neoplasms veterinary, Papilloma veterinary, Papillomaviridae immunology, Papillomavirus Infections veterinary, Tumor Virus Infections veterinary, Warts veterinary

Abstract

Papillomaviruses occasionally cause severe, nonregressing or recurrent infections in their human and animal hosts. The mechanisms underlying these atypical infections are not known. Canine oral papillomavirus (COPV) typically regresses spontaneously and is an important model of mucosal human papillomavirus infections. A severe, naturally occurring, nonregressing COPV infection provided an opportunity to investigate some aspects of viral pathogenicity and host immunity. In this case, the papillomas proved refractory to surgical and medical treatments, including autogenous vaccination and vaccination with capsid (L1) virus-like particles. High levels of induced anti-L1 antibodies appeared to have no effect on the infection. The papillomas spread to oesophageal mucosa, perioral haired skin, and remote cutaneous sites. Isolation of COPV from the animal and sequencing of several regions of the viral genome showed no differences to the COPV prototype. Experimental infection of beagle dogs with this viral isolate resulted in the uncomplicated development and regression of oral warts within the usual period, indicating that the virus was not an unusual pathogenic variant. These findings support the hypothesis that the recurrent lesions seen in some human papillomavirus infections, such as recurrent laryngeal papillomatosis, are associated with specific defects in host immunity rather than variations in viral pathogenicity., (Copyright 1999 Academic Press.)

Published

1999