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Microbiology | 1987

Immunoprotective Human Monoclonal Antibodies against Five Major Serotypes of Pseudomonas aeruginosa

Shuzo Sawada; Takashi Kawamura; Yasuhiko Masuho

Human monoclonal antibodies (Mabs) against the O antigens of Pseudomonas aeruginosa lipopolysaccharides (LPS) were produced by cell fusion between human tonsillar lymphocytes and P3-X63-Ag8-U1 (P3U1) mouse myeloma cells. To obtain human Mabs efficiently, 6 d culture supernatants of pokeweed-mitogen-stimulated lymphocytes (21 cultures from peripheral blood and 76 from tonsils) were assayed by ELISA. Five tonsillar lymphocytes which produced IgG antibody specific for P. aeruginosa LPS were preselected for fusion. The human Mabs, named P1-1 (IgG2, kappa), P5-1 (IgG2, lambda), P7-1 (IgG2, lambda), P8-1 (IgG2, lambda) and P10-1 (IgG2, kappa), bound with high specificity to Homma standard serotype strains A, E, B, G and I, respectively, and recognized O antigens. Each Mab showed opsonophagocytic killing activity of the corresponding serotype strain. Four of the Mabs caused agglutination at a very low concentration; a rather higher concentration of P7-1 was required for this effect. Although all the Mabs conferred type-specific protection against peritoneal infection, the strongly agglutinating Mabs provided better protection than the moderately agglutinating P7-1. The protective activity of P8-1 was estimated in compromised mice. A low dose (PD50 0.5-0.6 microgram per mouse) of P8-1 prevented subcutaneous infection in burned mice and peritoneal infection in leucopenic mice. All the hybridomas described here could be cultured in serum-free medium, and they have continued to secrete human Mabs for more than 14 months at rates of 10-20 micrograms per 10(6) cells in 24 h. These results suggested that these five human Mabs specific for O antigens might be useful in the prophylaxis and treatment of P. aeruginosa infections.


Biochemical and Biophysical Research Communications | 1986

Generation of hybridomas producing human monoclonal antibodies against herpes simplex virus after invitro stimulation

Yasuhiko Masuho; Tohru Sugano; Yoh-Ichi Matsumoto; Shuzo Sawada; Katsuhiko Tomibe

Hybridomas producing human monoclonal antibodies against herpes simplex virus were generated by in vitro antigen stimulation before cell fusion. The cell fusion with tonsillar lymphocytes which were stimulated with antigen and/or pokeweed mitogen generated many hybridomas producing human IgG against the virus. A combination of antigen and pokeweed mitogen synergistically enhanced the generation of virus-specific hybridomas. Furthermore, the higher the antibody response of the tonsil, the more virus-specific hybridomas were generated by the cell fusion. These results suggest that cell fusion with in vitro stimulated lymphocytes can be applied to a variety of clinically relevant viruses.


The Journal of Infectious Diseases | 1984

Protection Against Infection with Pseudomonas aeruginosa by Passive Transfer of Monoclonal Antibodies to Lipopolysaccharides and Outer Membrane Proteins

Shuzo Sawada; Masahiko Suzuki; Takashi Kawamura; Shigeki Fujinaga; Yasuhiko Masuho; Katsuhiko Tomibe


FEBS Journal | 1987

Characterization of a polysaccharide component of lipopolysaccharide from Pseudomonas aeruginosa IID 1008 (ATCC 27584) as D-rhamnan

Shin-ichi Yokota; Shuzo Sawada; Takashi Kawamura; Yoshio Araki; Eiji Ito


The Journal of Infectious Diseases | 1985

Characterization of a Human Monoclonal Antibody to Lipopolysaccharides of Pseudomonas aeruginosa Serotype 5: A Possible Candidate as an Immunotherapeutic Agent for Infections with P. aeruginosa

Shuzo Sawada; Takashi Kawamura; Yasuhiko Masuho; Katsuhiko Tomibe


The Journal of Infectious Diseases | 1985

A New Common Polysaccharide Antigen of Strains of Pseudomonas aeruginosa Detected with a Monoclonal Antibody

Shuzo Sawada; Takashi Kawamura; Yasuhiko Masuho; Katsuhiko Tomibe


Archive | 1985

Anti-pseudomonas aeruginosa human monoclonal antibody

Shuzo Sawada; Takashi Kawamura; Yasuhiko Masuho; Katsuhiko Tomibe


Archive | 1986

E87ag antigen of pseudomonas aeruginosa, monoclonal antibody against it, and hybridoma

Shuzo Sawada; Takashi Kawamura; Yasuhiko Masuho; Katsuhiko Tomibe


Archive | 1981

IgM Derivatives and process for the preparation thereof

Shuzi Miura; Tsunemasa Yoshida; Shoji Ono; Yasuhiko Masuho; Shuzo Sawada


Archive | 1990

E87AG ANTIGENS OF PSEUDOMONAS AERUGINOSA AND MONOCLONAL ANTIBODIES AGAINST THEM AND HYBRIDOMAS THEREOF

Shuzo Sawada; Takashi Kawamura; Yasuhiko Masuho; Katsuhiko Tomibe

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Yasuhiko Masuho

Tokyo University of Science

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