Atypical B cells (CD21-CD27-IgD-) correlate with lack of response to checkpoint inhibitor therapy in NSCLC

R. A. Belderbos, O. B. J. Corneth, D. Dumoulin, R. W. Hendriks,J. G. J. V. Aerts, M. Willemsen

EUROPEAN JOURNAL OF CANCER(2024)

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摘要
Introduction: Checkpoint inhibitor (CI) therapy has revolutionized treatment for non-small cell lung cancer (NSCLC). However, a proportion of patients do not respond to CI therapy for unknown reasons. Although the current paradigm in anti-tumor immunity evolves around T cells, the presence of tertiary lymphoid structures and memory B cells has been positively correlated with response to CI therapy in NSCLC. In addition, double negative (DN) (CD27- IgD-) B cells have been shown to be abundant in NSCLC compared to healthy lung tissue and inversely correlate with the intratumoral presence of memory B cells. Nonetheless, no study has correlated DN B cells to survival in NSCLC.Methods: In this study, we evaluated the presence and phenotype of B cells in peripheral blood with flow cytometry of patients with NSCLC and mesothelioma before receiving CI therapy and correlated these with clinical outcome.Results: Non-responding patients showed decreased frequencies of B cells, yet increased frequencies of antigen-experienced CD21-DN (Atypical) B cells compared to responding patients and HC, which was confirmed in patients with mesothelioma treated with CI therapy. Conclusions: These data show that the frequency of CD21-DN B cells correlates with lack of response to CI therapy in thoracic malignancies. The mechanism by which CD21-DN B cells hamper CI therapy remains un-known. Our findings support the hypothesis that CD21-DN B cells resemble phenotypically identical exhausted B cells that are seen in chronic infection or function as antigen presenting cells that induce regulatory T cells.
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关键词
Atypical B cells,B lymphocytes,Immune checkpoint inhibitors,NSCLC,MPM
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