Temperature-sensitive mutants of Actinobacillus pleuropneumoniae 4074, serotype 1, were isolated after treatment with nitrosoguanidine and enrichment with penicillin and D-cycloserine. Of the four temperature- sensitive mutants evaluated in mice, one (A-1) had a tight phenotype (i.e., it ceased replication immediately after transfer to the nonpermissive temperature [37°C]) and three (1-2, 4-1, and 12-1) were coasters that continued replication for up to three generations after transfer to 37°C. The reversion frequencies ranged from 10-6 to 10-9, and cutoff temperatures ranged from 33 tn 35°C. No major changes were detected in the biochemical profiles; agglutination reactions; electrophoretic profiles of the lipopolysaccharides, outer membrane proteins, and hemolysin proteins; hemolytic titers; or CAMP factor reactions of the mutants and the wild-type bacteria. Groups of 3- to 5-week-old, female ICR mice were immunized intranasally with three doses of 3.5 x 106 CFU of the mutants over 3 weeks and subsequently challenged intranasally with 5 50% lethal doses of the parental wild-type. Protection was induced by both the tight and the coaster mutants, with the 4-1 and 12-1 coasters eliciting greater protection (67 and 82%, respectively) than that induced by the A-1 light mutant (57%). Intranasal immunization with both phenotypes induced serum antibody responses against the surface antigens and the hemolysin protein.
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Byrd, W., & Hooke, A. M. (1997). Temperature-sensitive mutants of Actinobacillus pleuropneumoniae induce protection in mice. Infection and Immunity, 65(6), 2206–2210. https://doi.org/10.1128/iai.65.6.2206-2210.1997