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Featured researches published by K Hatano.


Infection and Immunity | 2002

Construction and Characterization of a Live, Attenuated aroA Deletion Mutant of Pseudomonas aeruginosa as a Candidate Intranasal Vaccine

Gregory P. Priebe; Mary M. Brinig; K Hatano; Martha Grout; Fadie T. Coleman; Gerald B. Pier; Joanna B. Goldberg

ABSTRACT Antibodies to the lipopolysaccharide O antigen of Pseudomonas aeruginosa mediate high-level immunity, but protective epitopes have proven to be poorly immunogenic, while nonprotective or minimally protective O-antigen epitopes often elicit the best immune responses. With the goal of developing a broadly protective P. aeruginosa vaccine, we used a gene replacement system based on the Flp recombinase to construct an unmarked aroA deletion mutant of the P. aeruginosa serogroup O2/O5 strain PAO1. The resultant aroA deletion mutant of PAO1 is designated PAO1ΔaroA. The aroA deletion was confirmed by both PCR and failure of the mutant to grow on minimal media lacking aromatic amino acids. When evaluated for safety and immunogenicity in mice, PAO1ΔaroA could be applied either intranasally or intraperitoneally at doses up to 5 × 109 CFU per mouse without adverse effects. No dissemination of PAO1ΔaroA to blood, liver, or spleen was detected after intranasal application, and histological evidence of pneumonia was minimal. Intranasal immunization of mice and rabbits elicited high titers of immunoglobulin G to whole bacterial cells and to heat-stable bacterial antigens of all seven prototypic P. aeruginosa serogroup O2/O5 strains. The mouse antisera mediated potent phagocytic killing of most of the prototypic serogroup O2/O5 strains, while the rabbit antisera mediated phagocytic killing of several serogroup-heterologous strains in addition to killing all O2/O5 strains. This live, attenuated P. aeruginosa strain PAO1ΔaroA appears to be safe for potential use as an intranasal vaccine and elicits high titers of opsonic antibodies against multiple strains of the P. aeruginosa O2/O5 serogroup.


Journal of Bacteriology | 1999

Characterization of the serogroup O11 O-antigen locus of Pseudomonas aeruginosa PA103

Charles R. Dean; C V Franklund; J. D. Retief; Michael J. Coyne; K Hatano; David J. Evans; Gerald B. Pier; J B Goldberg


Journal of Bacteriology | 1993

Synthesis of lipopolysaccharide O side chains by Pseudomonas aeruginosa PAO1 requires the enzyme phosphomannomutase

J B Goldberg; K Hatano; Gerald B. Pier


Proceedings of the National Academy of Sciences of the United States of America | 1992

Cloning and surface expression of Pseudomonas aeruginosa O antigen in Escherichia coli.

Joanna B. Goldberg; K Hatano; G S Meluleni; Gerald B. Pier


FEBS Journal | 2001

Structural analysis of the lipopolysaccharide core of a rough, cystic fibrosis isolate of Pseudomonas aeruginosa

Yuriy A. Knirel; Ol’ga V. Bystrova; Alexander S. Shashkov; Buko Lindner; Nina A. Kocharova; Sof’ya N. Senchenkova; Hermann Moll; Ulrich Zähringer; K Hatano; Gerald B. Pier


Infection and Immunity | 1998

Complex Serology and Immune Response of Mice to Variant High-Molecular-Weight O Polysaccharides Isolated from Pseudomonas aeruginosa Serogroup O2 Strains

K Hatano; Gerald B. Pier


Infection and Immunity | 1995

Biologic activities of antibodies to the neutral-polysaccharide component of the Pseudomonas aeruginosa lipopolysaccharide are blocked by O side chains and mucoid exopolysaccharide (alginate).

K Hatano; Joanna B. Goldberg; Gerald B. Pier


Infection and Immunity | 1994

Immunogenic and antigenic properties of a heptavalent high-molecular-weight O-polysaccharide vaccine derived from Pseudomonas aeruginosa.

K Hatano; Saskia Boisot; D DesJardins; D C Wright; J Brisker; Gerald B. Pier


Journal of Bacteriology | 1993

Pseudomonas aeruginosa lipopolysaccharide: evidence that the O side chains and common antigens are on the same molecule.

K Hatano; J B Goldberg; Gerald B. Pier


Journal of Biological Chemistry | 1989

The structure and serologic distribution of an extracellular neutral polysaccharide from Pseudomonas aeruginosa immunotype 3.

Nina A. Kocharova; K Hatano; A S Shaskov; Yuriy A. Knirel; N. K. Kochetkov; Gerald B. Pier

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Gerald B. Pier

Brigham and Women's Hospital

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J B Goldberg

Brigham and Women's Hospital

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Nina A. Kocharova

Russian Academy of Sciences

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Yuriy A. Knirel

Russian Academy of Sciences

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Buko Lindner

University of California

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David J. Evans

University of California

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Gloria Meluleni

Brigham and Women's Hospital

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