Osteopontin is a Therapeutic Target That Drives Breast Cancer Recurrence

Overview

Journal Nat Commun

Specialty Biology

Date 2024 Oct 25

PMID 39448577

Authors

Yu Gu

Tarek Taifour

Tung Bui

Dongmei Zuo

Alain Pacis

Alexandre Poirier

Sherif Attalla

Anne-Marie Fortier

Virginie Sanguin-Gendreau

Tien-Chi Pan

Vasilios Papavasiliou

Nancy U Lin

Melissa E Hughes

Kalie Smith

Morag Park

Michel L Tremblay

Lewis A Chodosh

Rinath Jeselsohn

William J Muller

Affiliations

Soon will be listed here.

Abstract

Recurrent breast cancers often develop resistance to standard-of-care therapies. Identifying targetable factors contributing to cancer recurrence remains the rate-limiting step in improving long-term outcomes. In this study, we identify tumor cell-derived osteopontin as an autocrine and paracrine driver of tumor recurrence. Osteopontin promotes tumor cell proliferation, recruits macrophages, and synergizes with IL-4 to further polarize them into a pro-tumorigenic state. Macrophage depletion and osteopontin inhibition decrease recurrent tumor growth. Furthermore, targeting osteopontin in primary tumor-bearing female mice prevents metastasis, permits T cell infiltration and activation, and improves anti-PD-1 immunotherapy response. Clinically, osteopontin expression is higher in recurrent metastatic tumors versus female patient-matched primary breast tumors. Osteopontin positively correlates with macrophage infiltration, increases with higher tumor grade, and its elevated pathway activity is associated with poor prognosis and long-term recurrence. Our findings suggest clinical implications and an alternative therapeutic strategy based on osteopontin's multiaxial role in breast cancer progression and recurrence.

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