Tumor-educated B cells selectively promote breast cancer lymph node metastasis by HSPA4-targeting IgG

被引:0
|
作者
Yan Gu
Yanfang Liu
Li Fu
Lili Zhai
Jie Zhu
Yanmei Han
Yingming Jiang
Yi Zhang
Peng Zhang
Zhengping Jiang
Xiang Zhang
Xuetao Cao
机构
[1] Second Military Medical University,National Key Laboratory of Medical Immunology & Institute of Immunology
[2] Second Military Medical University,Department of Pathology, Changhai Hospital
[3] Cancer Hospital,Department of Breast Cancer Pathology and Research Laboratory
[4] Tianjin Medical University,Department of Immunology & Center for Immunotherapy, Institute of Basic Medical Sciences, Peking Union Medical College
[5] Chinese Academy of Medical Sciences,College of Life Science
[6] Nankai University,undefined
来源
Nature Medicine | 2019年 / 25卷
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摘要
Primary tumors may create the premetastatic niche in secondary organs for subsequent metastasis. Humoral immunity contributes to the progression of certain cancers, but the roles of B cells and their derived antibodies in premetastatic niche formation are poorly defined. Using a mouse model of spontaneous lymph node metastasis of breast cancer, we show that primary tumors induced B cell accumulation in draining lymph nodes. These B cells selectively promoted lymph node metastasis by producing pathogenic IgG that targeted glycosylated membrane protein HSPA4, and activated the HSPA4-binding protein ITGB5 and the downstream Src/NF-κB pathway in tumor cells for CXCR4/SDF1α-axis-mediated metastasis. High serum anti-HSPA4 IgG was correlated with high tumor HSPA4 expression and poor prognosis of breast cancer subjects. Our findings identify a key role for tumor-educated B cells and their derived antibodies in lymph node premetastatic niche formation, providing potential targets for cancer intervention.
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页码:312 / 322
页数:10
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