跳轉至內容
Merck
  • ANGPTL2 increases bone metastasis of breast cancer cells through enhancing CXCR4 signaling.

ANGPTL2 increases bone metastasis of breast cancer cells through enhancing CXCR4 signaling.

Scientific reports (2015-03-17)
Tetsuro Masuda, Motoyoshi Endo, Yutaka Yamamoto, Haruki Odagiri, Tsuyoshi Kadomatsu, Takayuki Nakamura, Hironori Tanoue, Hitoshi Ito, Masaki Yugami, Keishi Miyata, Jun Morinaga, Haruki Horiguchi, Ikuyo Motokawa, Kazutoyo Terada, Masaki Suimye Morioka, Ichiro Manabe, Hirotaka Iwase, Hiroshi Mizuta, Yuichi Oike
摘要

Bone metastasis of breast cancer cells is a major concern, as it causes increased morbidity and mortality in patients. Bone tissue-derived CXCL12 preferentially recruits breast cancer cells expressing CXCR4 to bone metastatic sites. Thus, understanding how CXCR4 expression is regulated in breast cancer cells could suggest approaches to decrease bone metastasis of breast tumor cells. Here, we show that tumor cell-derived angiopoietin-like protein 2 (ANGPTL2) increases responsiveness of breast cancer cells to CXCL12 by promoting up-regulation of CXCR4 in those cells. In addition, we used a xenograft mouse model established by intracardiac injection of tumor cells to show that ANGPTL2 knockdown in breast cancer cells attenuates tumor cell responsiveness to CXCL12 by decreasing CXCR4 expression in those cells, thereby decreasing bone metastasis. Finally, we found that ANGPTL2 and CXCR4 expression levels within primary tumor tissues from breast cancer patients are positively correlated. We conclude that tumor cell-derived ANGPTL2 may increase bone metastasis by enhancing breast tumor cell responsiveness to CXCL12 signaling through up-regulation of tumor cell CXCR4 expression. These findings may suggest novel therapeutic approaches to treat metastatic breast cancer.

材料
產品編號
品牌
產品描述

Sigma-Aldrich
细胞计数试剂盒 - 8, for quantitation of viable cell number in proliferation and cytotoxicity assays