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Dive into the research topics where Brian Dizon is active.

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Featured researches published by Brian Dizon.


Proceedings of the National Academy of Sciences of the United States of America | 2012

Altered Ig levels and antibody responses in mice deficient for the Fc receptor for IgM (FcμR)

Kazuhito Honjo; Yoshiki Kubagawa; Dewitt Jones; Brian Dizon; Zilu Zhu; Hiroshi Ohno; Shozo Izui; John F. Kearney; Hiromi Kubagawa

Cell surface Fc receptor for IgM antibody (FcμR) is the most recently identified member among FcRs. We determined the cellular distribution of mouse FcμR and the functional consequences of Fcmr disruption. Surface FcμR expression was restricted to B-lineage cells, from immature B to plasma cells, except for a transient down-modulation during germinal center reactions. Fcmr ablation had no significant effect on overall B- and T-cell development, but led to a reduction of marginal zone B cells and an increase in splenic B1 B cells. Preimmune serum IgM in mutant mice was significantly elevated as were natural autoantibodies. When immunized with live attenuated pneumococci, mutant mice mounted robust antibody responses against phosphorylcholine, but not protein, determinants compared with wild-type mice. By contrast, upon immunization with a hapten-carrier conjugate, nitrophenyl-coupled chicken γ-globulin (NP-CGG), the mutant mice had a diminished primary IgG1 response to both NP and CGG. These findings suggest that FcμR has an important role in IgM homeostasis and regulation of humoral immune responses.


Journal of Immunology | 2008

Cathelicidin administration protects mice from Bacillus anthracis spore challenge.

Mark W. Lisanby; Melissa Swiecki; Brian Dizon; Kathryn J. Pflughoeft; Theresa M. Koehler; John F. Kearney

Cathelicidins are a family of cationic peptides expressed in mammals that possess numerous bactericidal and immunomodulatory properties. In vitro analyses showed that human, mouse, and pig cathelicidins inhibited Bacillus anthracis bacterial growth at micromolar concentrations in the presence or absence of capsule. Combined in vitro analyses of the effects of each peptide on spore germination and vegetative outgrowth by time lapse phase contrast microscopy, transmission electron microscopy, and flow cytometric analysis showed that only the pig cathelicidin was capable of directly arresting vegetative outgrowth and killing the developing bacilli within the confines of the exosporium. C57BL/6 mice were protected from spore-induced death by each cathelicidin in a time- and dose-dependent manner. Protection afforded by the porcine cathelicidin was due to its bactericidal effects, whereas the human and mouse cathelicidins appeared to mediate protection through increased recruitment of neutrophils to the site of infection. These findings suggest that cathelicidins might be utilized to augment the initial innate immune response to B. anthracis spore exposure and prevent the development of anthrax.


Journal of Immunology | 2012

Antibodies Generated against Conserved Antigens Expressed by Bacteria and Allergen-Bearing Fungi Suppress Airway Disease

Nicholas W. Kin; Emily K. Stefanov; Brian Dizon; John F. Kearney

There has been a sharp rise in allergic asthma and asthma-related deaths in the developed world, in contrast to many childhood illnesses that have been reduced or eliminated. The hygiene hypothesis proposes that excessively sanitary conditions early in life result in autoimmune and allergic phenomena because of a failure of the immune system to receive proper microbial stimulation during development. We demonstrate that Abs generated against conserved bacterial polysaccharides are reactive with and dampen the immune response against chitin and Aspergillus fumigatus. A reduction in Ag uptake, cell influx, cell activation, and cytokine production occurred in the presence of anti-polysaccharide Abs, resulting in a striking decrease in the severity of allergic airway disease in mice. Overall, our results suggest that Ag exposure—derived from environmental sources, self-antigens, or vaccination—during the neonatal period has dramatic effects on the adult Ab response and modifies the development of allergic airway disease.


Journal of Immunology | 2016

Effects of neonatal antigen exposure on natural antibody repertoire development

James New; Brian Dizon; R. Glenn King; John F. Kearney


Journal of Immunology | 2015

Modulation of autoimmune diabetes by innate-like B cell derived antibodies specific for N-acetyl-D-glucosamine. (BA7P.148)

James New; Brian Dizon; R. King; John F. Kearney


Journal of Immunology | 2012

Antibodies generated against conserved antigens suppress allergic airway disease

Emily K. Stefanov; Nicolas Kin; Brian Dizon; John F. Kearney


Journal of Immunology | 2012

Anti-Group B streptococci Ib antibodies protect against invasive aspergillosis.

Rebekah Wharton; Brian Dizon; John F. Kearney


Journal of Immunology | 2012

Altered humoral immune responses in mice deficient for the Fc receptor for IgM (Fc{mu}R)

Kazuhito Honjo; Yoshiki Kubagawa; Dewitt Jones; Brian Dizon; Hiroshi Ohno; John F. Kearney; Hiromi Kubagawa


Journal of Immunology | 2011

Modulation of autoimmune diabetes by antibodies specific for N-acetyl-D-glucosamine (P4026)

Brian Dizon; Neil S. Greenspan; John F. Kearney


Journal of Immunology | 2011

Group B streptococci Ib monoclonal antibodies protect against invasive aspergillosis.

Rebekah Wharton; Brian Dizon; John F. Kearney

Collaboration


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John F. Kearney

University of Alabama at Birmingham

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Dewitt Jones

University of Alabama at Birmingham

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Emily K. Stefanov

University of Alabama at Birmingham

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Hiromi Kubagawa

University of Alabama at Birmingham

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James New

University of Alabama at Birmingham

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Kazuhito Honjo

University of Alabama at Birmingham

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Neil S. Greenspan

Case Western Reserve University

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Rebekah Wharton

University of Alabama at Birmingham

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Yoshiki Kubagawa

University of Alabama at Birmingham

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Hiroshi Ohno

Yokohama City University

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