Estrogen-dependent DLL1-mediated Notch Signaling Promotes Luminal Breast Cancer

Overview

Journal Oncogene

Specialties Molecular Biology
Oncology

Date 2018 Nov 17

PMID 30442981

Citations 49

Authors

Sushil Kumar

Ratnesh Kumar Srivastav

David W Wilkes

Taylor Ross

Sabrina Kim

Jules Kowalski

Srinivas Chatla

Qing Zhang

Anupma Nayak

Manti Guha

Serge Y Fuchs

Christoforos Thomas

Rumela Chakrabarti

Affiliations

Soon will be listed here.

Abstract

Aberrant Notch signaling is implicated in several cancers, including breast cancer. However, the mechanistic details of the specific receptors and function of ligand-mediated Notch signaling that promote breast cancer remains elusive. In our studies we show that DLL1, a Notch signaling ligand, is significantly overexpressed in ERα luminal breast cancer. Intriguingly, DLL1 overexpression correlates with poor prognosis in ERα luminal breast cancer, but not in other subtypes of breast cancer. In addition, this effect is specific to DLL1, as other Notch ligands (DLL3, JAGGED1, and JAGGED2) do not influence the clinical outcome of ERα patients. Genetic studies show that DLL1-mediated Notch signaling in breast cancer is important for tumor cell proliferation, angiogenesis, and cancer stem cell function. Consistent with prognostic clinical data, we found the tumor-promoting function of DLL1 is exclusive to ERα luminal breast cancer, as loss of DLL1 inhibits both tumor growth and lung metastasis of luminal breast cancer. Importantly, we find that estrogen signaling stabilizes DLL1 protein by preventing its proteasomal and lysososmal degradations. Moreover, estrogen inhibits ubiquitination of DLL1. Together, our results highlight an unexpected and novel subtype-specific function of DLL1 in promoting luminal breast cancer that is regulated by estrogen signaling. Our studies also emphasize the critical role of assessing subtype-specific mechanisms driving tumor growth and metastasis to generate effective subtype-specific therapeutics.

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