Masami Yayoshi scite author profile

Masami Yayoshi

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Urawa University

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Relationship between an 85 kDa Protein and the Protective Effects of Mycoplasma pneumoniae

Yayoshi

Sasaki

Yoshioka³

1992

Microbiology and Immunology

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In the immunoblot analysis, sera from patients infected with Mycoplasma pneumoniae reacted with the 168 kDa (P1) and the 85 kDa proteins of virulent strain FH-P24 and P24-S1 mutant strain but not with the 85 kDa protein of P24-S11. Sera of hamsters and BALB/c mice, which had been immunized with live vaccines, were tested. In FH-P24 immunized animals, 100% or 80%, and in P24-S1, 40% of hamsters and 60% of BALB/c mice, developed antibodies against the 85 kDa protein, but antibodies were not detected in sera of P24-S11 immunized animals. The correlation between the development of antibodies to 85 kDa protein in the sera of vaccinated animals and the effects of protection by living vaccines were suggested.Mycoplasma pneumoniae is a major cause of epidemic nonviral pneumonia in children and young adults. An effective vaccine against M. pneumoniae disease would therefore be desirable.There have been three basic approaches to vaccine development, a whole-cell formalin-inactivated vaccine (22,23,25), a live attenuated vaccine (4, 11, 12) and a purified component vaccine (3,5,6). A single dose of inactivated vaccine has only a minimal protective effect. Multiple doses of vaccine containing adjuvant protect hamsters. The protective effect of inactivated vaccine was dose-dependent (1). Live vaccines composed of M. pneumoniae strains attenuated by continuous passages in vitro or temperature-sensitive mutants protected hamsters, but are unsuitable for human use because they retained partial virulence or decreased immunogenicity (4, 12). A current approach to vaccine development is based on producing cell extract vaccines made of defined cell components of the pathogen (5-7), especially the disease-related and virulence-related antigenic components, such as the attachment protein P1 (17, 18). It is not clear whether a vaccine made entirely of the P1 protein would be effective in protection against M. pneumoniae disease.We previously isolated nonhemolysis mutants of M. pneumoniae FH-P24 by the nitrosoguanidine (NTG) method (31, 32). Two of those mutants, P24-S1 and P24-S11, lost the virulence to golden hamsters. Only P24-S1 live vaccine showed protectivity in hamsters and BALB/c mice (33, 34) . The antibody, especially of 455

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Masami Yayoshi

Relationship between an 85 kDa Protein and the Protective Effects of Mycoplasma pneumoniae

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