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Aberrant high expression of immunoglobulin G in epithelial stem/progenitor-like cells contributes to tumor initiation and metastasis
Author(s) -
Qinyuan Liao,
Wei Liu,
Yang Liu,
Fulin Wang,
Chong Wang,
Jingxuan Zhang,
Ming Chu,
Dongyang Jiang,
Lin Xiao,
Wenwei Shao,
Zhengzuo Sheng,
Tao Xia,
Lei Huo,
C. Cameron Yin,
Youhui Zhang,
Gregory Lee,
Jing Huang,
Zihai Li,
Xiaoyan Qiu
Publication year - 2015
Publication title -
oncotarget
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.373
H-Index - 127
ISSN - 1949-2553
DOI - 10.18632/oncotarget.5542
Subject(s) - metastasis , cancer research , cancer stem cell , progenitor cell , stem cell , biology , cancer cell , cancer , immunoglobulin superfamily , immunology , antibody , microbiology and biotechnology , genetics
High expression of immunoglobulin G (IgG) in many non-B cell malignancies and its non-conventional roles in promoting proliferation and survival of cancer cells have been demonstrated. However, the precise function of non-B IgG remains incompletely understood. Here we define the antigen specificity of RP215, a monoclonal antibody that specifically recognizes the IgG in cancer cells. Using RP215, our study shows that IgG is overexpressed in cancer cells of epithelial lineage, especially cells with cancer stem/progenitor cell-like features. The RP215-recognized IgG is primarily localized on the cell surface, particularly lamellipodia-like structures. Cells with high IgG display higher migration, increased invasiveness and metastasis, and enhanced self-renewal and tumorgenecity ability in vitro and in vivo. Importantly, depletion of IgG in breast cancer leads to reduced adhesion, invasion and self-renewal and increased apoptosis of cancer cells. We conclude that high expression of IgG is a novel biomarker of tumor progression, metastasis and cancer stem cell maintenance and demonstrate the potential therapeutic benefits of RP215-recognized IgG targeted strategy.

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