NF kappa B regulator Bcl3 controls development and function of classical dendritic cells required for resistance to Toxoplasma gondii

The atypical IκB family member Bcl3 associates with p50/NF-κB1 or p52/NF-κB2 homodimers in the nucleus, and positively or negatively modulates transcription in a context-dependent manner. In mice lacking Bcl3 globally or specifically in CD11c(+) cells, we previously reported that Toxoplasma gondii i...

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Autores principales: Guha, June, Kang, Byunghyun, Claudio, Estefania, Redekar, Neelam R., Wang, Hongshan, Kelsall, Brian L., Siebenlist, Ulrich, Murphy, Philip M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9651595/
https://www.ncbi.nlm.nih.gov/pubmed/36318581
http://dx.doi.org/10.1371/journal.ppat.1010502
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author Guha, June
Kang, Byunghyun
Claudio, Estefania
Redekar, Neelam R.
Wang, Hongshan
Kelsall, Brian L.
Siebenlist, Ulrich
Murphy, Philip M.
author_facet Guha, June
Kang, Byunghyun
Claudio, Estefania
Redekar, Neelam R.
Wang, Hongshan
Kelsall, Brian L.
Siebenlist, Ulrich
Murphy, Philip M.
author_sort Guha, June
collection PubMed
description The atypical IκB family member Bcl3 associates with p50/NF-κB1 or p52/NF-κB2 homodimers in the nucleus, and positively or negatively modulates transcription in a context-dependent manner. In mice lacking Bcl3 globally or specifically in CD11c(+) cells, we previously reported that Toxoplasma gondii infection is uniformly fatal and is associated with an impaired Th1 immune response. Since Bcl3 expression in dendritic cells (DC) is pivotal for antigen presentation and since classical DCs (cDC) are major antigen presenting cells, we investigated the role of Bcl3 specifically in cDCs in vivo by crossing Zbtb46 cre mice with Bcl3(flx/flx) mice. Bcl3(flx/flx) Zbtb46 cre mice were as susceptible to lethal T. gondii infection as total Bcl3(-/-) mice and generated poor Th1 immune responses. Consistent with this, compared to wildtype controls, splenic Xcr1(+) Bcl3-deficient cDC1 cells were defective in presenting Ova antigen to OT-I cells both for Ova(257-264) peptide and after infection with Ovalbumin-expressing T. gondii. Moreover, splenic CD4(+) and CD8(+) T cells from infected Bcl3(flx/flx) Zbtb46 cre mice exhibited decreased T. gondii-specific priming as revealed by both reduced cytokine production and reduced T. gondii-specific tetramer staining. In vitro differentiation of cDCs from bone marrow progenitors also revealed Bcl3-dependent cDC-specific antigen-presentation activity. Consistent with this, splenocyte single cell RNA seq (scRNAseq) in infected mice revealed Bcl3-dependent expression of genes involved in antigen processing in cDCs. We also identified by scRNAseq, a unique Bcl3-dependent hybrid subpopulation of Zbtb46(+) DCs co-expressing the monocyte/macrophage transcription factor Lysozyme M. This subpopulation exhibited Bcl3-dependent expansion after infection. Likewise, by flow cytometry we identified two T. gondii-induced hybrid subpopulations of Bcl3-dependent cDC1 and cDC2 cells both expressing monocyte/macrophage markers, designated as icDC1 and icDC2. Together, our results indicate that Bcl3 in classical DCs is a major determinant of protective T cell responses and survival in T. gondii-infection.
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spelling pubmed-96515952022-11-15 NF kappa B regulator Bcl3 controls development and function of classical dendritic cells required for resistance to Toxoplasma gondii Guha, June Kang, Byunghyun Claudio, Estefania Redekar, Neelam R. Wang, Hongshan Kelsall, Brian L. Siebenlist, Ulrich Murphy, Philip M. PLoS Pathog Research Article The atypical IκB family member Bcl3 associates with p50/NF-κB1 or p52/NF-κB2 homodimers in the nucleus, and positively or negatively modulates transcription in a context-dependent manner. In mice lacking Bcl3 globally or specifically in CD11c(+) cells, we previously reported that Toxoplasma gondii infection is uniformly fatal and is associated with an impaired Th1 immune response. Since Bcl3 expression in dendritic cells (DC) is pivotal for antigen presentation and since classical DCs (cDC) are major antigen presenting cells, we investigated the role of Bcl3 specifically in cDCs in vivo by crossing Zbtb46 cre mice with Bcl3(flx/flx) mice. Bcl3(flx/flx) Zbtb46 cre mice were as susceptible to lethal T. gondii infection as total Bcl3(-/-) mice and generated poor Th1 immune responses. Consistent with this, compared to wildtype controls, splenic Xcr1(+) Bcl3-deficient cDC1 cells were defective in presenting Ova antigen to OT-I cells both for Ova(257-264) peptide and after infection with Ovalbumin-expressing T. gondii. Moreover, splenic CD4(+) and CD8(+) T cells from infected Bcl3(flx/flx) Zbtb46 cre mice exhibited decreased T. gondii-specific priming as revealed by both reduced cytokine production and reduced T. gondii-specific tetramer staining. In vitro differentiation of cDCs from bone marrow progenitors also revealed Bcl3-dependent cDC-specific antigen-presentation activity. Consistent with this, splenocyte single cell RNA seq (scRNAseq) in infected mice revealed Bcl3-dependent expression of genes involved in antigen processing in cDCs. We also identified by scRNAseq, a unique Bcl3-dependent hybrid subpopulation of Zbtb46(+) DCs co-expressing the monocyte/macrophage transcription factor Lysozyme M. This subpopulation exhibited Bcl3-dependent expansion after infection. Likewise, by flow cytometry we identified two T. gondii-induced hybrid subpopulations of Bcl3-dependent cDC1 and cDC2 cells both expressing monocyte/macrophage markers, designated as icDC1 and icDC2. Together, our results indicate that Bcl3 in classical DCs is a major determinant of protective T cell responses and survival in T. gondii-infection. Public Library of Science 2022-11-01 /pmc/articles/PMC9651595/ /pubmed/36318581 http://dx.doi.org/10.1371/journal.ppat.1010502 Text en https://creativecommons.org/publicdomain/zero/1.0/This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 (https://creativecommons.org/publicdomain/zero/1.0/) public domain dedication.
spellingShingle Research Article
Guha, June
Kang, Byunghyun
Claudio, Estefania
Redekar, Neelam R.
Wang, Hongshan
Kelsall, Brian L.
Siebenlist, Ulrich
Murphy, Philip M.
NF kappa B regulator Bcl3 controls development and function of classical dendritic cells required for resistance to Toxoplasma gondii
title NF kappa B regulator Bcl3 controls development and function of classical dendritic cells required for resistance to Toxoplasma gondii
title_full NF kappa B regulator Bcl3 controls development and function of classical dendritic cells required for resistance to Toxoplasma gondii
title_fullStr NF kappa B regulator Bcl3 controls development and function of classical dendritic cells required for resistance to Toxoplasma gondii
title_full_unstemmed NF kappa B regulator Bcl3 controls development and function of classical dendritic cells required for resistance to Toxoplasma gondii
title_short NF kappa B regulator Bcl3 controls development and function of classical dendritic cells required for resistance to Toxoplasma gondii
title_sort nf kappa b regulator bcl3 controls development and function of classical dendritic cells required for resistance to toxoplasma gondii
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9651595/
https://www.ncbi.nlm.nih.gov/pubmed/36318581
http://dx.doi.org/10.1371/journal.ppat.1010502
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