Malaria infection alters the expression of B-cell activating factor resulting in diminished memory antibody responses and survival
Malaria is a major cause of morbidity worldwide with reports of over 200-500 million infected individuals and nearly 1 million deaths each year. Antibodies have been shown to play a critical role in controlling the blood stage of this disease; however, in malaria-endemic areas antibody immunity is s...
Published in: | European Journal of Immunology |
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2012
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ftunivqespace:oai:espace.library.uq.edu.au:UQ:289337 2023-05-15T15:35:27+02:00 Malaria infection alters the expression of B-cell activating factor resulting in diminished memory antibody responses and survival Liu, Xue Q. Stacey, Katryn J. Horne-Debets, Joshua M. Cridland, Jasmyn A. Fischer, Katja Narum, David Mackay, Fabienne Pierce, Susan K. Wykes, Michelle N. 2012-12-01 https://espace.library.uq.edu.au/view/UQ:289337 eng eng Wiley - V C H Verlag doi:10.1002/eji.201242689 issn:0014-2980 issn:1521-4141 orcid:0000-0002-3992-7802 Baffin-island DCS Malaria Memory B cells 2403 Immunology 2723 Immunology and Allergy Journal Article 2012 ftunivqespace https://doi.org/10.1002/eji.201242689 2020-12-07T23:51:40Z Malaria is a major cause of morbidity worldwide with reports of over 200-500 million infected individuals and nearly 1 million deaths each year. Antibodies have been shown to play a critical role in controlling the blood stage of this disease; however, in malaria-endemic areas antibody immunity is slow to develop despite years of exposure to Plasmodium spp. the causative parasite. Using rodent Plasmodium yoelii YM, we provide evidence that malarial infections result in a decrease in the proportion of DCs that express the B-cell survival factor, BAFF, resulting in a decreased ability of these DCs to support memory B-cell differentiation into antibody secreting cells (ASCs) and/or the survival of ASCs. Further, compared with infected WT mice, ASC numbers were significantly increased in malaria-infected transgenic mice that either overexpressed BAFF or mice with BAFF-independent B-cell survival (B-cell-restricted TRAF3 deletion). Remarkably, BAFF-overexpressing mice were protected from lethal malaria infections, indicating the significance of the role BAFF plays in determining the outcome of malaria infections. These findings describe a previously unappreciated mechanism by which Plasmodium spp. can depress the generation of protective antibody responses. Article in Journal/Newspaper Baffin Island Baffin The University of Queensland: UQ eSpace Baffin Island European Journal of Immunology 42 12 3291 3301 |
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Open Polar |
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The University of Queensland: UQ eSpace |
op_collection_id |
ftunivqespace |
language |
English |
topic |
Baffin-island DCS Malaria Memory B cells 2403 Immunology 2723 Immunology and Allergy |
spellingShingle |
Baffin-island DCS Malaria Memory B cells 2403 Immunology 2723 Immunology and Allergy Liu, Xue Q. Stacey, Katryn J. Horne-Debets, Joshua M. Cridland, Jasmyn A. Fischer, Katja Narum, David Mackay, Fabienne Pierce, Susan K. Wykes, Michelle N. Malaria infection alters the expression of B-cell activating factor resulting in diminished memory antibody responses and survival |
topic_facet |
Baffin-island DCS Malaria Memory B cells 2403 Immunology 2723 Immunology and Allergy |
description |
Malaria is a major cause of morbidity worldwide with reports of over 200-500 million infected individuals and nearly 1 million deaths each year. Antibodies have been shown to play a critical role in controlling the blood stage of this disease; however, in malaria-endemic areas antibody immunity is slow to develop despite years of exposure to Plasmodium spp. the causative parasite. Using rodent Plasmodium yoelii YM, we provide evidence that malarial infections result in a decrease in the proportion of DCs that express the B-cell survival factor, BAFF, resulting in a decreased ability of these DCs to support memory B-cell differentiation into antibody secreting cells (ASCs) and/or the survival of ASCs. Further, compared with infected WT mice, ASC numbers were significantly increased in malaria-infected transgenic mice that either overexpressed BAFF or mice with BAFF-independent B-cell survival (B-cell-restricted TRAF3 deletion). Remarkably, BAFF-overexpressing mice were protected from lethal malaria infections, indicating the significance of the role BAFF plays in determining the outcome of malaria infections. These findings describe a previously unappreciated mechanism by which Plasmodium spp. can depress the generation of protective antibody responses. |
format |
Article in Journal/Newspaper |
author |
Liu, Xue Q. Stacey, Katryn J. Horne-Debets, Joshua M. Cridland, Jasmyn A. Fischer, Katja Narum, David Mackay, Fabienne Pierce, Susan K. Wykes, Michelle N. |
author_facet |
Liu, Xue Q. Stacey, Katryn J. Horne-Debets, Joshua M. Cridland, Jasmyn A. Fischer, Katja Narum, David Mackay, Fabienne Pierce, Susan K. Wykes, Michelle N. |
author_sort |
Liu, Xue Q. |
title |
Malaria infection alters the expression of B-cell activating factor resulting in diminished memory antibody responses and survival |
title_short |
Malaria infection alters the expression of B-cell activating factor resulting in diminished memory antibody responses and survival |
title_full |
Malaria infection alters the expression of B-cell activating factor resulting in diminished memory antibody responses and survival |
title_fullStr |
Malaria infection alters the expression of B-cell activating factor resulting in diminished memory antibody responses and survival |
title_full_unstemmed |
Malaria infection alters the expression of B-cell activating factor resulting in diminished memory antibody responses and survival |
title_sort |
malaria infection alters the expression of b-cell activating factor resulting in diminished memory antibody responses and survival |
publisher |
Wiley - V C H Verlag |
publishDate |
2012 |
url |
https://espace.library.uq.edu.au/view/UQ:289337 |
geographic |
Baffin Island |
geographic_facet |
Baffin Island |
genre |
Baffin Island Baffin |
genre_facet |
Baffin Island Baffin |
op_relation |
doi:10.1002/eji.201242689 issn:0014-2980 issn:1521-4141 orcid:0000-0002-3992-7802 |
op_doi |
https://doi.org/10.1002/eji.201242689 |
container_title |
European Journal of Immunology |
container_volume |
42 |
container_issue |
12 |
container_start_page |
3291 |
op_container_end_page |
3301 |
_version_ |
1766365782883696640 |