Back to Search Start Over

Notch promotes recurrence of dormant tumor cells following HER2/neu-targeted therapy

Authors :
Abravanel, Daniel L.
Belka, George K.
Pan, Tien-chi
Pant, Dhruv K.
Collins, Meredith A.
Sterner, Christopher J.
Chodosh, Lewis A.
Source :
Journal of Clinical Investigation. July, 2015, Vol. 125 Issue 7, p2484, 13 p.
Publication Year :
2015

Abstract

Breast cancer mortality is principally due to recurrent tumors that arise from a reservoir of residual tumor cells that survive therapy. Remarkably, breast cancers can recur after extended periods of clinical remission, implying that at least some residual tumor cells pass through a dormant phase prior to relapse. Nevertheless, the mechanisms that contribute to breast cancer recurrence are poorly understood. Using a mouse model of recurrent mammary tumorigenesis in combination with bioinformatics analyses of breast cancer patients, we have identified a role for Notch signaling in mammary tumor dormancy and recurrence. Specifically, we found that Notch signaling is acutely upregulated in tumor cells following HER2/neu pathway inhibition, that Notch signaling remains activated in a subset of dormant residual tumor cells that persist following HER2/ neu downregulation, that activation of Notch signaling accelerates tumor recurrence, and that inhibition of Notch signaling by either genetic or pharmacological approaches impairs recurrence in mice. Consistent with these findings, meta- analysis of microarray data from over 4,000 breast cancer patients revealed that elevated Notch pathway activity is independently associated with an increased rate of recurrence. Together, these results implicate Notch signaling in tumor recurrence from dormant residual tumor cells and provide evidence that dormancy is a targetable stage of breast cancer progression.<br />Introduction Improvements in the early detection of breast cancers--coupled with advances in surgery, radiotherapy, and adjuvant therapy--have led to substantial increases in 5-year survival rates for breast cancer patients over [...]

Details

Language :
English
ISSN :
00219738
Volume :
125
Issue :
7
Database :
Gale General OneFile
Journal :
Journal of Clinical Investigation
Publication Type :
Academic Journal
Accession number :
edsgcl.421907166
Full Text :
https://doi.org/10.1172/Jci74883