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B lymphocytes can be activated to act as antigen presenting cells to promote anti-tumor responses

CD80 CD40 CD86 抗原提呈细胞 免疫系统 人口 免疫学 抗原 T细胞 树突状细胞 生物 癌症研究 细胞毒性T细胞 医学 体外 生物化学 环境卫生
作者
Renata Ariza Marques Rossetti,Noely Paula Cristina Lorenzi,Kaori Yokochi,Maria Beatriz Sartor de Faria Rosa,Luciana Benevides,Paulo Francisco Ramos Margarido,Edmund Chada Baracat,Jesus Paula Carvalho,Luisa L. Villa,Ana Paula Lepique
出处
期刊:PLOS ONE [Public Library of Science]
卷期号:13 (7): e0199034-e0199034 被引量:92
标识
DOI:10.1371/journal.pone.0199034
摘要

Immune evasion by tumors includes several different mechanisms, including the inefficiency of antigen presenting cells (APCs) to trigger anti-tumor T cell responses. B lymphocytes may display a pro-tumoral role but can also be modulated to function as antigen presenting cells to T lymphocytes, capable of triggering anti-cancer immune responses. While dendritic cells, DCs, are the best APC population to activate naive T cells, DCs or their precursors, monocytes, are frequently modulated by tumors, displaying a tolerogenic phenotype in cancer patients. In patients with cervical cancer, we observed that monocyte derived DCs are tolerogenic, inhibiting allogeneic T cell activation compared to the same population obtained from patients with precursor lesions or cervicitis. In this work, we show that B lymphocytes from cervical cancer patients respond to treatment with sCD40L and IL-4 by increasing the CD80+CD86+ population, therefore potentially increasing their ability to activate T cells. To test if B lymphocytes could actually trigger anti-tumor T cell responses, we designed an experimental model where we harvested T and B lymphocytes, or dendritic cells, from tumor bearing donors, and after APC stimulation, transplanted them, together with T cells into RAG1-/- recipients, previously injected with tumor cells. We were able to show that anti-CD40 activated B lymphocytes could trigger secondary T cell responses, dependent on MHC-II expression. Moreover, we showed that dendritic cells were resistant to the anti-CD40 treatment and unable to stimulate anti-tumor responses. In summary, our results suggest that B lymphocytes may be used as a tool for immunotherapy against cancer.

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