Browsing by Author "Li, Ping"
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Item Src Inhibition Blocks c-Myc Translation and Glucose Metabolism to Prevent the Development of Breast Cancer(AACR, 2015) Jain, Shalini; Wang, Xiao; Chang, Chia-Chi; Ibarra-Drendall, Catherine; Wang, Hai; Zhang, Qingling; Brady, Samuel W.; Li, Ping; Zhao, Hong; Dobbs, Jessica; Kyrish, Matt; Tkaczyk, Tomasz S.; Ambrose, Adrian; Sistrunk, Christopher; Arun, Banu K.; Richards-Kortum, Rebecca; Jia, Wei; Seewaldt, Victoria L.; Yu, Dihua; BioengineeringPreventing breast cancer will require the development of targeted strategies that can effectively block disease progression. Tamoxifen and aromatase inhibitors are effective in addressing estrogen receptor–positive (ER+) breast cancer development, but estrogen receptor–negative (ER−) breast cancer remains an unmet challenge due to gaps in pathobiologic understanding. In this study, we used reverse-phase protein array to identify activation of Src kinase as an early signaling alteration in premalignant breast lesions of women who did not respond to tamoxifen, a widely used ER antagonist for hormonal therapy of breast cancer. Src kinase blockade with the small-molecule inhibitor saracatinib prevented the disorganized three-dimensional growth of ER− mammary epithelial cells in vitro and delayed the development of premalignant lesions and tumors in vivo in mouse models developing HER2+ and ER− mammary tumors, extending tumor-free and overall survival. Mechanistic investigations revealed that Src blockade reduced glucose metabolism as a result of an inhibition in ERK1/2–MNK1–eIF4E–mediated cap-dependent translation of c-Myc and transcription of the glucose transporter GLUT1, thereby limiting energy available for cell growth. Taken together, our results provide a sound rationale to target Src pathways in premalignant breast lesions to limit the development of breast cancers.