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Published in: Tumor Biology 1/2016

01-01-2016 | Original Article

Adaptive B cell responses in rituximab-treated diffuse large B cell lymphoma patients during complete remission

Authors: Zhanshan Cha, Chen Li, Yan Zang, Haihui Gu, Huijun Guo, Jinqi Li, Yuan Fang, Thomas F. Petersen, Jing Li, Richard O. Karas, Michele L. Hamilton, Baohua Qian

Published in: Tumor Biology | Issue 1/2016

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Abstract

Rituximab is a chimeric monoclonal antibody directed against the CD20 antigen. Treatment using rituximab in combination with chemotherapy has dramatically improved overall survival rate of diffuse large B cell lymphoma (DLBCL). Since rituximab can deplete both lymphoma B cells and normal B cells, how rituximab-treatment affects normal B cell function in DLBCL patients under remission is unclear. Here, we examined peripheral blood B cell composition and antigen-specific B cell responses in DLBCL patients in remission and observed reductions in the frequencies of total B cell as well as several major B cell subsets, including CD19+IgD+ naive B cells, CD19+IgDCD27+ memory B cells, and CD19loCD27hi plasmablasts. Moreover, tetanus toxin (TT)-specific B cell proliferation was reduced in DLBCL patients in remission. On the other hand, HA-specific IgG-secreting B cell responses could be stimulated by influenza vaccination in DLBCL patients in remission, demonstrating that the machinery for generating de novo adaptive B cell responses was functional in DLBCL patients in remission. Our results provided insights in normal B cell function in DLBCL patients in remission.
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Metadata
Title
Adaptive B cell responses in rituximab-treated diffuse large B cell lymphoma patients during complete remission
Authors
Zhanshan Cha
Chen Li
Yan Zang
Haihui Gu
Huijun Guo
Jinqi Li
Yuan Fang
Thomas F. Petersen
Jing Li
Richard O. Karas
Michele L. Hamilton
Baohua Qian
Publication date
01-01-2016
Publisher
Springer Netherlands
Published in
Tumor Biology / Issue 1/2016
Print ISSN: 1010-4283
Electronic ISSN: 1423-0380
DOI
https://doi.org/10.1007/s13277-015-3872-6

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