Your search keyword '"Williamson, E.D."' showing total 3 results

1. Conjugation of Y. pestis F1-antigen to gold nanoparticles improves immunogenicity

Author

Gregory, A.E., Williamson, E.D., Prior, J.L., Butcher, W.A., Thompson, I.J., Shaw, A.M., and Titball, R.W.

Subjects

*BIOCONJUGATES, *YERSINIA pestis, *ANTIGENS, *IMMUNOGENETICS, *GOLD nanoparticles, *LABORATORY mice, *COUPLING agents (Chemistry), *IMMUNOGLOBULIN G

Abstract

Abstract: The efficacy of 15nm gold nanoparticles (AuNP) coated with Yersinia pestis F1-antigen, as an immunogen in mice, has been assessed. The nanoparticles were decorated with F1-antigen using N-hydroxysuccinimide and N-(3-dimethylaminopropyl)-N′-ethylcarbodiimide hydrochloride coupling chemistry. Mice given AuNP-F1 in alhydrogel generated the greatest IgG antibody response to F1-antigen when compared with mice given AuNP-F1 in PBS or given unconjugated F1-antigen in PBS or alhydrogel. Compared with unconjugated F1-antigen, the IgG2a response was enhanced in mice dosed with AuNP-F1 in PBS (p <0.05) but not in mice immunised with AuNP-F1 in alhydrogel. All treatment groups developed a memory response to F1-antigen, the polarity of which was inflenced by formulation in alhydrogel. The sera raised against F1-antigen coupled to AuNPs was able to competitively bind to rF1-antigen, displacing protective macaque sera. [Copyright &y& Elsevier]

Published

2012

2. Kinetics of the immune response to the (F1+V) vaccine in models of bubonic and pneumonic plague

Author

Williamson, E.D., Stagg, A.J., Eley, S.M., Taylor, R., Green, M., Jones, S.M., and Titball, R.W.

Subjects

*PREVENTIVE medicine, *VACCINATION, *ENTEROBACTERIACEAE, *IMMUNOGLOBULIN G

Abstract

Abstract: Protection against aerosol challenge with >300MLD of Yersinia pestis was observed 7 days after a single immunisation of mice with the F1+V vaccine. At day 60, mice were protected against injected challenge (107 MLD) in a vaccine dose-related manner. Recall responses to rV in splenocytes ex vivo at day 98 correlated significantly (p <0.001) with the immunising dose-level of V antigen; no memory response or anti-V serum IgG was detected in killed whole cell vaccine (KWCV) recipients. This may explain the susceptibility of KWCV recipients to aerosol challenge and the enhanced protection conferred by the F1+V sub-unit vaccine, particularly since the anti-F1 responses induced by either vaccine were similarly IgG1-polarised. [Copyright &y& Elsevier]

Published

2007

3. Immunogenicity of the rF1+rV vaccine for plague with identification of potential immune correlates

Author

Williamson, E.D., Flick-Smith, H.C., Waters, E., Miller, J., Hodgson, I., Le Butt, C.S., and Hill, J.

Subjects

*IMMUNOGLOBULIN G, *PREVENTIVE medicine, *SERUM, *BLOOD plasma

Abstract

Abstract: The rF1+rV candidate sub-unit vaccine for plague, formulated by adsorption to alhydrogel, has been demonstrated to be immunogenic in the cynomolgus macaque in a clinically relevant dose-range (5–40μg of each sub-unit) and regimen. Following two doses of vaccine, a specific IgG titre developed in a dose-related manner with predominance of the IgG1/IgG2 isotypes. Groups of macaques receiving only a single dose of vaccine at the 40μg dose-level had a significantly reduced peak IgG response and faster decline to baseline. Serum collected at week 5 from 19 immunised animals competed with and displaced murine Mab7.3 from binding to the V antigen in vitro. By week 53 of the schedule, although absolute IgG titres had declined, 17/19 macaque sera tested contained competing antibody, indicating the durability of a functional immune response to rF1+rV in this species. Thirteen of these week 53 sera were passively transferred into groups of naive mice, and all conferred full or partial protection against subsequent challenge of the mice with plague. Generally, those sera which were most competitive with Mab 7.3 for binding to V antigen were fully protective by passive transfer, although one week-53 serum sample was fully protective by passive transfer but not active by competitive ELISA. The early development of protective immunity in macaques was also indicated from the protection conferred on naive mice by the passive transfer of immune macaque serum collected at 2–10 weeks of the immunisation schedule. Serum samples from representative macaques within this time period also inhibited the Yersinia-mediated cytotoxicity of J774 macrophages in a qualitative in vitro assay of type three secretion. [Copyright &y& Elsevier]

Published

2007