Molecular correlates of response to eribulin and pembrolizumab in hormone receptor-positive metastatic breast cancer

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作者
Tanya E. Keenan
Jennifer L. Guerriero
Romualdo Barroso-Sousa
Tianyu Li
Tess O’Meara
Anita Giobbie-Hurder
Nabihah Tayob
Jiani Hu
Mariano Severgnini
Judith Agudo
Ines Vaz-Luis
Leilani Anderson
Victoria Attaya
Jihye Park
Jake Conway
Meng Xiao He
Brendan Reardon
Erin Shannon
Gerburg Wulf
Laura M. Spring
Rinath Jeselsohn
Ian Krop
Nancy U. Lin
Ann Partridge
Eric P. Winer
Elizabeth A. Mittendorf
David Liu
Eliezer M. Van Allen
Sara M. Tolaney
机构
[1] Dana-Farber Cancer Institute,Department of Medical Oncology
[2] Broad Institute of Massachusetts Institute of Technology and Harvard,Breast Oncology Program
[3] Dana-Farber/Brigham and Women’s Cancer Center,Breast Tumor Immunology Laboratory, Department of Cancer Biology
[4] Dana-Farber Cancer Institute,Division of Breast Surgery, Department of Surgery
[5] Brigham and Women’s Hospital,Ludwig Center for Cancer Research at Harvard
[6] Harvard Medical School,Oncology Center
[7] Hospital Sírio-Libanês,Division of Biostatistics, Department of Data Sciences
[8] Dana-Farber Cancer Institute,Center for Immuno
[9] Boston,Oncology
[10] Dana-Farber Cancer Institute,Department of Cancer Immunology and Virology
[11] Dana-Farber Cancer Institute,Medical Oncology Department, INSERM Unit 981, Molecular Predictors and New Targets in Oncology
[12] Institut Gustave Roussy,Hematology/Oncology
[13] Harvard Graduate Program in Biophysics,Breast Cancer, Cancer Center
[14] Beth Israel Deaconess Medical Center,undefined
[15] Massachusetts General Hospital,undefined
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摘要
Immune checkpoint inhibitors (ICIs) have minimal therapeutic effect in hormone receptor-positive (HR+ ) breast cancer. We present final overall survival (OS) results (n = 88) from a randomized phase 2 trial of eribulin ± pembrolizumab for patients with metastatic HR+ breast cancer, computationally dissect genomic and/or transcriptomic data from pre-treatment tumors (n = 52) for molecular associations with efficacy, and identify cytokine changes differentiating response and ICI-related toxicity (n = 58). Despite no improvement in OS with combination therapy (hazard ratio 0.95, 95% CI 0.59–1.55, p = 0.84), immune infiltration and antigen presentation distinguished responding tumors, while tumor heterogeneity and estrogen signaling independently associated with resistance. Moreover, patients with ICI-related toxicity had lower levels of immunoregulatory cytokines. Broadly, we establish a framework for ICI response in HR+ breast cancer that warrants diagnostic and therapeutic validation. ClinicalTrials.gov Registration: NCT03051659.
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