Inflammatory B cells correlate with failure to checkpoint blockade in melanoma patients
The understanding of the role of B cells in patients with solid tumors remains insufficient. We found that circulating B cells produced TNFα and/or IL-6, associated with unresponsiveness and poor overall survival of melanoma patients treated with anti-CTLA4 antibody. Transcriptome analysis of B cell...
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Online Access: | http://dx.doi.org/10.1080/2162402X.2021.1873585 |
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doaj-00b74b7d42214ef4aec781fbe3b69ef92021-02-08T14:09:16ZengTaylor & Francis GroupOncoImmunology2162-402X2021-01-0110110.1080/2162402X.2021.18735851873585Inflammatory B cells correlate with failure to checkpoint blockade in melanoma patientsKaat de Jonge0Laure Tillé1Joao Lourenco2Hélène Maby-El Hajjami3Sina Nassiri4Julien Racle5David Gfeller6Mauro Delorenzi7Grégory Verdeil8Petra Baumgaertner9Daniel E. Speiser10University of LausanneUniversity of LausanneSIB Swiss Institute of BioinformaticsUniversity of LausanneUniversity of LausanneUniversity of LausanneUniversity of LausanneSIB Swiss Institute of BioinformaticsUniversity of LausanneUniversity of LausanneUniversity of LausanneThe understanding of the role of B cells in patients with solid tumors remains insufficient. We found that circulating B cells produced TNFα and/or IL-6, associated with unresponsiveness and poor overall survival of melanoma patients treated with anti-CTLA4 antibody. Transcriptome analysis of B cells from melanoma metastases showed enriched expression of inflammatory response genes. Publicly available single B cell data from the tumor microenvironment revealed a negative correlation between TNFα expression and response to immune checkpoint blockade. These findings suggest that B cells contribute to tumor growth via the production of inflammatory cytokines. Possibly, these B cells are different from tertiary lymphoid structure-associated B cells, which have been described to correlate with favorable clinical outcome of cancer patients. Further studies are required to identify and characterize B cell subsets and their functions promoting or counteracting tumor growth, with the aim to identify biomarkers and novel treatment targets.http://dx.doi.org/10.1080/2162402X.2021.1873585b cellstumor microenvironmentimmune checkpointmelanomainflammation |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Kaat de Jonge Laure Tillé Joao Lourenco Hélène Maby-El Hajjami Sina Nassiri Julien Racle David Gfeller Mauro Delorenzi Grégory Verdeil Petra Baumgaertner Daniel E. Speiser |
spellingShingle |
Kaat de Jonge Laure Tillé Joao Lourenco Hélène Maby-El Hajjami Sina Nassiri Julien Racle David Gfeller Mauro Delorenzi Grégory Verdeil Petra Baumgaertner Daniel E. Speiser Inflammatory B cells correlate with failure to checkpoint blockade in melanoma patients OncoImmunology b cells tumor microenvironment immune checkpoint melanoma inflammation |
author_facet |
Kaat de Jonge Laure Tillé Joao Lourenco Hélène Maby-El Hajjami Sina Nassiri Julien Racle David Gfeller Mauro Delorenzi Grégory Verdeil Petra Baumgaertner Daniel E. Speiser |
author_sort |
Kaat de Jonge |
title |
Inflammatory B cells correlate with failure to checkpoint blockade in melanoma patients |
title_short |
Inflammatory B cells correlate with failure to checkpoint blockade in melanoma patients |
title_full |
Inflammatory B cells correlate with failure to checkpoint blockade in melanoma patients |
title_fullStr |
Inflammatory B cells correlate with failure to checkpoint blockade in melanoma patients |
title_full_unstemmed |
Inflammatory B cells correlate with failure to checkpoint blockade in melanoma patients |
title_sort |
inflammatory b cells correlate with failure to checkpoint blockade in melanoma patients |
publisher |
Taylor & Francis Group |
series |
OncoImmunology |
issn |
2162-402X |
publishDate |
2021-01-01 |
description |
The understanding of the role of B cells in patients with solid tumors remains insufficient. We found that circulating B cells produced TNFα and/or IL-6, associated with unresponsiveness and poor overall survival of melanoma patients treated with anti-CTLA4 antibody. Transcriptome analysis of B cells from melanoma metastases showed enriched expression of inflammatory response genes. Publicly available single B cell data from the tumor microenvironment revealed a negative correlation between TNFα expression and response to immune checkpoint blockade. These findings suggest that B cells contribute to tumor growth via the production of inflammatory cytokines. Possibly, these B cells are different from tertiary lymphoid structure-associated B cells, which have been described to correlate with favorable clinical outcome of cancer patients. Further studies are required to identify and characterize B cell subsets and their functions promoting or counteracting tumor growth, with the aim to identify biomarkers and novel treatment targets. |
topic |
b cells tumor microenvironment immune checkpoint melanoma inflammation |
url |
http://dx.doi.org/10.1080/2162402X.2021.1873585 |
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