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Effect of Subcutaneous Anti-CD20 Antibody-Mediated B Cell Depletion on Susceptibility to Pneumocystis Infection in Mice

Prior work has shown that parenterally administered anti-CD20 (5D2) inhibits CD4(+) T cell priming in response to challenge with Pneumocystis murina and predisposes to pneumonia. In this study, we investigated the effect of subcutaneous anti-CD20 antibody and Pneumocystis infection. In mice with pri...

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Autores principales: Dai, Guixiang, Noell, Kristin, Weckbecker, Gisbert, Kolls, Jay K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8103991/
https://www.ncbi.nlm.nih.gov/pubmed/33952667
http://dx.doi.org/10.1128/mSphere.01144-20
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author Dai, Guixiang
Noell, Kristin
Weckbecker, Gisbert
Kolls, Jay K.
author_facet Dai, Guixiang
Noell, Kristin
Weckbecker, Gisbert
Kolls, Jay K.
author_sort Dai, Guixiang
collection PubMed
description Prior work has shown that parenterally administered anti-CD20 (5D2) inhibits CD4(+) T cell priming in response to challenge with Pneumocystis murina and predisposes to pneumonia. In this study, we investigated the effect of subcutaneous anti-CD20 antibody and Pneumocystis infection. In mice with primary infection, anti-CD20 antibody treatment depleted both CD19(+) and CD27(+) CD19(+) cells but not T cells in the lung at days 14 and 28 after Pneumocystis inoculation. Although anti-CD20 antibody treatment impaired fungal clearance at day 14 postinfection, fungal burden in the lungs was substantially reduced at day 28 in both depleted and control mice in the low-dose group. Subcutaneous anti-CD20 antibody treatment did not alter antigen-specific serum immunoglobulin levels in mice compared with control mice, and there were no significant differences in the numbers of lung gamma interferon-positive (IFN-γ(+)) CD4(+), interleukin 4-positive (IL-4(+)) CD4(+), IL-5(+) CD4(+), and IL-17A(+) CD4(+) cells between depleted and control mice after infection. In mice with secondary infection, the lung fungal burden was comparable between depleted and control mice 14 days after reinfection. Low-dose subcutaneous anti-CD20 antibody treatment may delay fungal clearance, but it did not impair the ability of the host to clear Pneumocystis infection, irrespective of primary or secondary infection. IMPORTANCE Anti-CD20 antibody therapy is used for both cancer and autoimmune disease but has been shown to be associated with Pneumocystis pneumonia in humans. This study shows that low-dose subcutaneous anti-CD20 can modulate B cell populations without grossly perturbing fungal immunity against Pneumocystis lung infection.
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spelling pubmed-81039912021-05-21 Effect of Subcutaneous Anti-CD20 Antibody-Mediated B Cell Depletion on Susceptibility to Pneumocystis Infection in Mice Dai, Guixiang Noell, Kristin Weckbecker, Gisbert Kolls, Jay K. mSphere Research Article Prior work has shown that parenterally administered anti-CD20 (5D2) inhibits CD4(+) T cell priming in response to challenge with Pneumocystis murina and predisposes to pneumonia. In this study, we investigated the effect of subcutaneous anti-CD20 antibody and Pneumocystis infection. In mice with primary infection, anti-CD20 antibody treatment depleted both CD19(+) and CD27(+) CD19(+) cells but not T cells in the lung at days 14 and 28 after Pneumocystis inoculation. Although anti-CD20 antibody treatment impaired fungal clearance at day 14 postinfection, fungal burden in the lungs was substantially reduced at day 28 in both depleted and control mice in the low-dose group. Subcutaneous anti-CD20 antibody treatment did not alter antigen-specific serum immunoglobulin levels in mice compared with control mice, and there were no significant differences in the numbers of lung gamma interferon-positive (IFN-γ(+)) CD4(+), interleukin 4-positive (IL-4(+)) CD4(+), IL-5(+) CD4(+), and IL-17A(+) CD4(+) cells between depleted and control mice after infection. In mice with secondary infection, the lung fungal burden was comparable between depleted and control mice 14 days after reinfection. Low-dose subcutaneous anti-CD20 antibody treatment may delay fungal clearance, but it did not impair the ability of the host to clear Pneumocystis infection, irrespective of primary or secondary infection. IMPORTANCE Anti-CD20 antibody therapy is used for both cancer and autoimmune disease but has been shown to be associated with Pneumocystis pneumonia in humans. This study shows that low-dose subcutaneous anti-CD20 can modulate B cell populations without grossly perturbing fungal immunity against Pneumocystis lung infection. American Society for Microbiology 2021-05-05 /pmc/articles/PMC8103991/ /pubmed/33952667 http://dx.doi.org/10.1128/mSphere.01144-20 Text en Copyright © 2021 Dai et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Dai, Guixiang
Noell, Kristin
Weckbecker, Gisbert
Kolls, Jay K.
Effect of Subcutaneous Anti-CD20 Antibody-Mediated B Cell Depletion on Susceptibility to Pneumocystis Infection in Mice
title Effect of Subcutaneous Anti-CD20 Antibody-Mediated B Cell Depletion on Susceptibility to Pneumocystis Infection in Mice
title_full Effect of Subcutaneous Anti-CD20 Antibody-Mediated B Cell Depletion on Susceptibility to Pneumocystis Infection in Mice
title_fullStr Effect of Subcutaneous Anti-CD20 Antibody-Mediated B Cell Depletion on Susceptibility to Pneumocystis Infection in Mice
title_full_unstemmed Effect of Subcutaneous Anti-CD20 Antibody-Mediated B Cell Depletion on Susceptibility to Pneumocystis Infection in Mice
title_short Effect of Subcutaneous Anti-CD20 Antibody-Mediated B Cell Depletion on Susceptibility to Pneumocystis Infection in Mice
title_sort effect of subcutaneous anti-cd20 antibody-mediated b cell depletion on susceptibility to pneumocystis infection in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8103991/
https://www.ncbi.nlm.nih.gov/pubmed/33952667
http://dx.doi.org/10.1128/mSphere.01144-20
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