| Literature DB >> 25545618 |
Huimin Tao1, Lin Lu, Yang Xia, Fu Dai, Yi Wang, Yangyi Bao, Steven K Lundy, Fumito Ito, Qin Pan, Xiaolian Zhang, Fang Zheng, Guoshun Shu, Bingmu Fang, Jinhong Jiang, Jianchuang Xia, Shiang Huang, Qiao Li, Alfred E Chang.
Abstract
We have previously reported that adoptive transfer of tumor-draining lymph node (TDLN) B cells confers tumor regression in a spontaneous pulmonary metastasis mouse model of breast cancer. In this study, we identified IL-10-producing cells within these B cells, and found that IL-10 removal, either by using IL-10(-/-) TDLN B cells or by systemic neutralization of IL-10, significantly augmented the therapeutic efficacy of adoptively transferred TDLN B cells. Depletion of IL-10 in B-cell adoptive transfers significantly increased CTLs and B-cell activity of PBMCs and splenic cells in the recipient. Activated TDLN B cells express Fas ligand, which was further enhanced by coculture of these TDLN B cells with 4T1 tumor cells. Effector B cells killed tumor cells directly in vitro in an antigen specific and Fas ligand-dependent manner. Trafficking of TDLN B cells in vivo suggested that they were recruited to the tumor and lung as well as secondary lymphoid organs. These findings further define the biological function of antitumor effector B cells, which may offer alternative cellular therapies to cancer.Entities:
Keywords: Adoptive Immunotherapy; B cells; Cytotoxicity; Fas; IL-10; Tumor
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Year: 2015 PMID: 25545618 PMCID: PMC4414939 DOI: 10.1002/eji.201444625
Source DB: PubMed Journal: Eur J Immunol ISSN: 0014-2980 Impact factor: 5.532