Toxoplasma gondii antigens GRA1 (p24) and SAG1 (p30): A comparison of their stimulatory influence on T-cell activation and cytokine expression in in vitro cultures

The influence of recombinant cell surface SAG1 (rp30) and secretory GRA1 (rp24) antigens (Ag) on T-cell activation and cytokine induction in vitro was compared. T-cell activity and the level of IFN-γ, IL-10 and IL-12 expression in rp30-immunized T cells were considerably increased in the presence of...

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Main Authors: Kato, Morimasa, Claveria, Florencia G., Maki, Y., Tanaka, T., Suzuki, N., Nagasawa, Hideyuki
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Published: Animo Repository 2005
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Online Access:https://animorepository.dlsu.edu.ph/faculty_research/3400
https://animorepository.dlsu.edu.ph/context/faculty_research/article/4402/type/native/viewcontent/000084120.html
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spelling oai:animorepository.dlsu.edu.ph:faculty_research-44022022-08-13T03:23:06Z Toxoplasma gondii antigens GRA1 (p24) and SAG1 (p30): A comparison of their stimulatory influence on T-cell activation and cytokine expression in in vitro cultures Kato, Morimasa Claveria, Florencia G. Maki, Y. Tanaka, T. Suzuki, N. Nagasawa, Hideyuki The influence of recombinant cell surface SAG1 (rp30) and secretory GRA1 (rp24) antigens (Ag) on T-cell activation and cytokine induction in vitro was compared. T-cell activity and the level of IFN-γ, IL-10 and IL-12 expression in rp30-immunized T cells were considerably increased in the presence of rp30 Ags. IgG2a and IgG1 antibodies (Ab) were detected in sera of rp24- and rp30-immunized mice, with the secretory rp24 Ag having induced significantly higher titer of IgG1 Ab. In vitro, the greater antigenicity of surface rp30 Ag was notable based on the level of T-cell activation, and cytokine synthesis suggestive of the participation of Th1 cells. Although, IFN-γ expression by rp24 Ag was lower compared to rp30 Ag, the synthesis of both IgG2a and IgG1 Abs reflects the protective nature of rp24 Ag. We have generated two recombinant Toxoplasma gondii Ags that demonstrated differences in antigenicity in vitro. It would be interesting to evaluate the mechanism(s) of immunity induced by SAG1 (p30) and GRA1 (p24) Ags against infection with T. gondii in vivo. Copyright © 2005 S. Karger AG. 2005-04-01T08:00:00Z text text/html https://animorepository.dlsu.edu.ph/faculty_research/3400 info:doi/10.1159/000084120 https://animorepository.dlsu.edu.ph/context/faculty_research/article/4402/type/native/viewcontent/000084120.html Faculty Research Work Animo Repository Toxoplasma gondii Antigens T cells Cytokines Biology
institution De La Salle University
building De La Salle University Library
continent Asia
country Philippines
Philippines
content_provider De La Salle University Library
collection DLSU Institutional Repository
topic Toxoplasma gondii
Antigens
T cells
Cytokines
Biology
spellingShingle Toxoplasma gondii
Antigens
T cells
Cytokines
Biology
Kato, Morimasa
Claveria, Florencia G.
Maki, Y.
Tanaka, T.
Suzuki, N.
Nagasawa, Hideyuki
Toxoplasma gondii antigens GRA1 (p24) and SAG1 (p30): A comparison of their stimulatory influence on T-cell activation and cytokine expression in in vitro cultures
description The influence of recombinant cell surface SAG1 (rp30) and secretory GRA1 (rp24) antigens (Ag) on T-cell activation and cytokine induction in vitro was compared. T-cell activity and the level of IFN-γ, IL-10 and IL-12 expression in rp30-immunized T cells were considerably increased in the presence of rp30 Ags. IgG2a and IgG1 antibodies (Ab) were detected in sera of rp24- and rp30-immunized mice, with the secretory rp24 Ag having induced significantly higher titer of IgG1 Ab. In vitro, the greater antigenicity of surface rp30 Ag was notable based on the level of T-cell activation, and cytokine synthesis suggestive of the participation of Th1 cells. Although, IFN-γ expression by rp24 Ag was lower compared to rp30 Ag, the synthesis of both IgG2a and IgG1 Abs reflects the protective nature of rp24 Ag. We have generated two recombinant Toxoplasma gondii Ags that demonstrated differences in antigenicity in vitro. It would be interesting to evaluate the mechanism(s) of immunity induced by SAG1 (p30) and GRA1 (p24) Ags against infection with T. gondii in vivo. Copyright © 2005 S. Karger AG.
format text
author Kato, Morimasa
Claveria, Florencia G.
Maki, Y.
Tanaka, T.
Suzuki, N.
Nagasawa, Hideyuki
author_facet Kato, Morimasa
Claveria, Florencia G.
Maki, Y.
Tanaka, T.
Suzuki, N.
Nagasawa, Hideyuki
author_sort Kato, Morimasa
title Toxoplasma gondii antigens GRA1 (p24) and SAG1 (p30): A comparison of their stimulatory influence on T-cell activation and cytokine expression in in vitro cultures
title_short Toxoplasma gondii antigens GRA1 (p24) and SAG1 (p30): A comparison of their stimulatory influence on T-cell activation and cytokine expression in in vitro cultures
title_full Toxoplasma gondii antigens GRA1 (p24) and SAG1 (p30): A comparison of their stimulatory influence on T-cell activation and cytokine expression in in vitro cultures
title_fullStr Toxoplasma gondii antigens GRA1 (p24) and SAG1 (p30): A comparison of their stimulatory influence on T-cell activation and cytokine expression in in vitro cultures
title_full_unstemmed Toxoplasma gondii antigens GRA1 (p24) and SAG1 (p30): A comparison of their stimulatory influence on T-cell activation and cytokine expression in in vitro cultures
title_sort toxoplasma gondii antigens gra1 (p24) and sag1 (p30): a comparison of their stimulatory influence on t-cell activation and cytokine expression in in vitro cultures
publisher Animo Repository
publishDate 2005
url https://animorepository.dlsu.edu.ph/faculty_research/3400
https://animorepository.dlsu.edu.ph/context/faculty_research/article/4402/type/native/viewcontent/000084120.html
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