Discrepancies in the tumor microenvironment of spontaneous and orthotopic murine models of pancreatic cancer uncover a new immunostimulatory phenotype for B cells
Discrepancies in the tumor microenvironment of spontaneous and orthotopic murine models of pancreatic cancer uncover a new immunostimulatory phenotype for B cells
B cells are salient features of pancreatic ductal adenocarcinoma (PDAC) tumors, yet their role in this disease remains controversial. Murine studies have indicated a protumoral role for B cells, whereas clinical data show tumor-infiltrating B cells are a positive prognostic factor, both in PDAC and other cancers. This disparity needs to be clarified in order to develop effective immunotherapies. In this study, we provide new evidence that reconcile human and mouse data and highlight the importance of using relevant preclinical tumor models when assessing B cell function. We compared B cell infiltration and activation in both a genetic model of murine PDAC (KPC mouse) and an injectable orthotopic model. A pronounced B cell infiltrate was only observed in KPC tumors and correlated with T cell infiltration, mirroring human disease. In contrast, orthotopic tumors exhibited a relative paucity of B cells. Accordingly, KPC-derived B cells displayed markers of B cell activation (germinal center entry, B cell memory, and plasma cell differentiation) accompanied by significant intratumoral immunoglobulin deposition, a feature markedly weaker in orthotopic tumors. Tumor immunoglobulins, however, did not appear to form immune complexes. Furthermore, in contrast to the current paradigm that tumor B cells are immunosuppressive, when assessed as a bulk population, intratumoral B cells upregulated several proinflammatory and immunostimulatory genes, a distinctly different phenotype to that of splenic-derived B cells; further highlighting the importance of studying tumor-infiltrating B cells over B cells from secondary lymphoid organs. In agreement with the current literature, genetic deletion of B cells (μMT mice) resulted in reduced orthotopic tumor growth, however, this was not recapitulated by treatment with B-cell-depleting anti-CD20 antibody and, more importantly, was not observed in anti-CD20-treated KPC mice. This suggests the result from B cell deficient mice might be caused by their altered immune system, rather than lack of B cells. Therefore, our data indicate B cells do not favor tumor progression. In conclusion, our analysis of relevant preclinical models shows B cells to be active members of the tumor microenvironment, producing immunostimulatory factors that might support the adaptive antitumor immune response, as suggested by human PDAC studies.
B cells, immunoglobulins, murine models, pancreatic cancer, tumor microenvironment
1-18
Spear, Sarah
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Candido, Juliana B.
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McDermott, Jacqueline R.
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Ghirelli, Cristina
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Maniati, Eleni
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Beers, Stephen A.
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Balkwill, Frances R.
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Kocher, Hemant M.
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Capasso, Melania
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27 March 2019
Spear, Sarah
86b87b51-3e4e-403b-9e02-093284173a5b
Candido, Juliana B.
cf0c9eca-df62-43a2-be64-b31aa8e3002e
McDermott, Jacqueline R.
364c2176-4180-4ffb-9698-4828be5c2e62
Ghirelli, Cristina
c465227b-7615-4f74-bdcf-61be850f92ad
Maniati, Eleni
c5554637-d56d-47f8-aee2-f8acdd70d09e
Beers, Stephen A.
a02548be-3ffd-41ab-9db8-d6e8c3b499a2
Balkwill, Frances R.
19bd5bcb-1698-43ee-b6c2-4c0912bd91a4
Kocher, Hemant M.
3523f9ee-b7a6-4b61-b231-8555585ab849
Capasso, Melania
b39e0740-6a4e-4133-b7ff-1900f8e6b9d0
Spear, Sarah, Candido, Juliana B., McDermott, Jacqueline R., Ghirelli, Cristina, Maniati, Eleni, Beers, Stephen A., Balkwill, Frances R., Kocher, Hemant M. and Capasso, Melania
(2019)
Discrepancies in the tumor microenvironment of spontaneous and orthotopic murine models of pancreatic cancer uncover a new immunostimulatory phenotype for B cells.
Frontiers in Immunology, 10 (542), .
(doi:10.3389/fimmu.2019.00542).
Abstract
B cells are salient features of pancreatic ductal adenocarcinoma (PDAC) tumors, yet their role in this disease remains controversial. Murine studies have indicated a protumoral role for B cells, whereas clinical data show tumor-infiltrating B cells are a positive prognostic factor, both in PDAC and other cancers. This disparity needs to be clarified in order to develop effective immunotherapies. In this study, we provide new evidence that reconcile human and mouse data and highlight the importance of using relevant preclinical tumor models when assessing B cell function. We compared B cell infiltration and activation in both a genetic model of murine PDAC (KPC mouse) and an injectable orthotopic model. A pronounced B cell infiltrate was only observed in KPC tumors and correlated with T cell infiltration, mirroring human disease. In contrast, orthotopic tumors exhibited a relative paucity of B cells. Accordingly, KPC-derived B cells displayed markers of B cell activation (germinal center entry, B cell memory, and plasma cell differentiation) accompanied by significant intratumoral immunoglobulin deposition, a feature markedly weaker in orthotopic tumors. Tumor immunoglobulins, however, did not appear to form immune complexes. Furthermore, in contrast to the current paradigm that tumor B cells are immunosuppressive, when assessed as a bulk population, intratumoral B cells upregulated several proinflammatory and immunostimulatory genes, a distinctly different phenotype to that of splenic-derived B cells; further highlighting the importance of studying tumor-infiltrating B cells over B cells from secondary lymphoid organs. In agreement with the current literature, genetic deletion of B cells (μMT mice) resulted in reduced orthotopic tumor growth, however, this was not recapitulated by treatment with B-cell-depleting anti-CD20 antibody and, more importantly, was not observed in anti-CD20-treated KPC mice. This suggests the result from B cell deficient mice might be caused by their altered immune system, rather than lack of B cells. Therefore, our data indicate B cells do not favor tumor progression. In conclusion, our analysis of relevant preclinical models shows B cells to be active members of the tumor microenvironment, producing immunostimulatory factors that might support the adaptive antitumor immune response, as suggested by human PDAC studies.
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fimmu-10-00542
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Accepted/In Press date: 28 February 2019
Published date: 27 March 2019
Keywords:
B cells, immunoglobulins, murine models, pancreatic cancer, tumor microenvironment
Identifiers
Local EPrints ID: 430742
URI: http://eprints.soton.ac.uk/id/eprint/430742
ISSN: 1664-3224
PURE UUID: 0acb080f-d332-4c3e-8c74-297a4d6ddc7a
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Date deposited: 10 May 2019 16:30
Last modified: 16 Mar 2024 03:18
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Contributors
Author:
Sarah Spear
Author:
Juliana B. Candido
Author:
Jacqueline R. McDermott
Author:
Cristina Ghirelli
Author:
Eleni Maniati
Author:
Frances R. Balkwill
Author:
Hemant M. Kocher
Author:
Melania Capasso
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