Author:
Dai Huijuan,Xu Wenting,Wang Lulu,Li Xiao,Sheng Xiaonan,Zhu Lei,Li Ye,Dong Xinrui,Zhou Weihang,Han Chenyu,Mao Yan,Yao Linli
Abstract
AbstractThe communication between tumor cells and tumor microenvironment plays a critical role in cancer development. Cancer-associated fibroblasts (CAFs) are the major components of the tumor microenvironment and take part in breast cancer formation and progression. Here, by comparing the gene expression patterns in CAFs and normal fibroblasts, we found SPRY2 expression was significantly decreased in CAFs and decreased SPRY2 expression was correlated with worse prognosis in breast cancer patients. SPRY2 knockdown in fibroblasts promoted tumor growth and distant metastasis of breast cancer in mice. Loss of stromal SPRY2 expression promoted CAF activation dependent on glycolytic metabolism. Mechanically, SPRY2 suppressed Y10 phosphorylation of LDHA and LDHA activity by interfering with the interaction between LDHA and SRC. Functionally, SPRY2 knockdown in fibroblasts enhanced the stemness of tumor cell dependent on glycolysis in fibroblasts. Collectively, this work identified SPRY2 as a negative regulator of CAF activation, and SPRY2 in CAFs may potentially be therapeutically targeted in breast cancer treatment.
Funder
Beijing Natural Science Foundation
Shanghai Municipal Health Commission
Shanghai Qingpu District Science and Technology Commission
National Natural Science Foundation of China
Natural Science Foundation of Shandong Municipality
Publisher
Springer Science and Business Media LLC