Safety and Protective Efficacy of Intramuscular Vaccination with a Live aroA Derivative of Pasteurella multocida B:2 against Experimental Hemorrhagic Septicemia in Calves

Author:

Dagleish Mark P.1,Hodgson J. Christopher1,Ataei Saeed2,Finucane Anna2,Finlayson Jeanie1,Sales Jill3,Parton Roger2,Coote John G.2

Affiliation:

1. Moredun Research Institute, International Research Centre, Pentlands Science Park, Bush Loan, Penicuik, Midlothian, United Kingdom

2. Infection and Immunity Division, Institute of Biomedical and Life Sciences, University of Glasgow, Glasgow, United Kingdom

3. Biomathematics & Statistics Scotland, James Clerk Maxwell Building, The King's Buildings, University of Edinburgh, Edinburgh, United Kingdom

Abstract

ABSTRACT Three groups of five calves, namely, V1, V2, and V3, were immunized intramuscularly at 4 and 8 weeks of age with ca. 10 9 , 10 8 , and 10 7 CFU, respectively, of a derivative of Pasteurella multocida B:2 wild-type strain 85020 containing a deletion in the aroA gene (strain JRMT12). The first and second vaccinations resulted in significantly ( P < 0.01) higher rectal temperature responses in groups V1 and V2 than in group V3. Serum immunoglobulin M (IgM) and IgG titers did not increase in any group until after the second vaccination and were then significantly higher in groups V1 and V2 than in group V3 ( P = 0.001 for both IgM and IgG). All vaccinated groups and three unvaccinated challenge control calves (group CC) were injected subcutaneously at 10 weeks of age with ca. 10 7 CFU of strain 85020. Vaccinated calves survived the challenge, but two CC animals developed clinical disease and were killed for humane reasons. After challenge, mean serum amyloid A concentrations were significantly higher ( P < 0.001) in the CC group than in the vaccinated groups. Postmortem examination revealed that calves in the CC group showed the most extensive range of bacteriologically positive tissues and gross and histopathological lesions. Overall, a clear dose-dependent response was present, with those receiving a higher vaccine dose being less affected clinically, bacteriologically, and pathologically by the wild-type challenge. The V2 treatment appeared to give the best combination of high immune response, protection, and safety.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Immunology,Microbiology,Parasitology

Reference25 articles.

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3. Carter, G. R., A. Myint, R. Vankhar, and A. Khin. 1991. Immunization of cattle and buffalos with live hemorrhagic septicemia vaccine. Vet. Rec.129:203.

4. Chandrasekaran, S., L. Kennett, P. C. Yeap, N. Muniandy, B. Rani, and T. K. S. Mukkur. 1994. Characterization of immune-response and duration of protection in buffalos immunized with hemorrhagic septicemia vaccines. Vet. Microbiol.41:213-219.

5. De Alwis, M. C. L. 1995. Haemorrhagic septicaemia (Pasteurella multocida serotype B:2 and E:2 infection) in cattle and buffaloes, p. 9-24. In W. Donachie, F. A. Lainson, and J. C. Hodgson (ed.), Haemophilus, Actinobacillus and Pasteurella. Plenum Press, New York, NY.

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