Bulk and Single-Cell Profiling of Breast Tumors Identifies TREM-1 as a Dominant Immune Suppressive Marker Associated With Poor Outcomes

Ashok K. Pullikuth; Eric D. Routh; Eric D. Routh; Kip D. Zimmerman; Julia Chifman; Julia Chifman; Jeff W. Chou; Jeff W. Chou; Michael H. Soike; Guangxu Jin; Guangxu Jin; Jing Su; Jing Su; Qianqian Song; Qianqian Song; Michael A. Black; Cristin Print; Davide Bedognetti; Marissa Howard-McNatt; Stacey S. O’Neill; Stacey S. O’Neill; Alexandra Thomas; Alexandra Thomas; Carl D. Langefeld; Carl D. Langefeld; Alexander B. Sigalov; Yong Lu; Yong Lu; Lance D. Miller; Lance D. Miller

doi:10.3389/fonc.2021.734959

Frontiers in Oncology (Dec 2021)

Bulk and Single-Cell Profiling of Breast Tumors Identifies TREM-1 as a Dominant Immune Suppressive Marker Associated With Poor Outcomes

Ashok K. Pullikuth,
Eric D. Routh,
Eric D. Routh,
Kip D. Zimmerman,
Julia Chifman,
Julia Chifman,
Jeff W. Chou,
Jeff W. Chou,
Michael H. Soike,
Guangxu Jin,
Guangxu Jin,
Jing Su,
Jing Su,
Qianqian Song,
Qianqian Song,
Michael A. Black,
Cristin Print,
Davide Bedognetti,
Marissa Howard-McNatt,
Stacey S. O’Neill,
Stacey S. O’Neill,
Alexandra Thomas,
Alexandra Thomas,
Carl D. Langefeld,
Carl D. Langefeld,
Alexander B. Sigalov,
Yong Lu,
Yong Lu,
Lance D. Miller,
Lance D. Miller

Affiliations

Ashok K. Pullikuth: Department of Cancer Biology, Wake Forest School of Medicine, Winston Salem, NC, United States
Eric D. Routh: Department of Cancer Biology, Wake Forest School of Medicine, Winston Salem, NC, United States
Eric D. Routh: Lineberger Comprehensive Cancer Center, University of North Carolina at Chapel Hill, Chapel Hill, NC, United States
Kip D. Zimmerman: Center for Precision Medicine, Wake Forest School of Medicine, Winston Salem, NC, United States
Julia Chifman: Department of Cancer Biology, Wake Forest School of Medicine, Winston Salem, NC, United States
Julia Chifman: Department of Mathematics and Statistics, American University, Washington, DC, United States
Jeff W. Chou: Department of Biostatistics and Data Science, Wake Forest School of Medicine, Winston Salem, NC, United States
Jeff W. Chou: The Comprehensive Cancer Center of Wake Forest University, Winston Salem, NC, United States
Michael H. Soike: Department of Radiation Oncology, University of Alabama-Birmingham, Birmingham, AL, United States
Guangxu Jin: Department of Cancer Biology, Wake Forest School of Medicine, Winston Salem, NC, United States
Guangxu Jin: The Comprehensive Cancer Center of Wake Forest University, Winston Salem, NC, United States
Jing Su: Department of Biostatistics and Data Science, Wake Forest School of Medicine, Winston Salem, NC, United States
Jing Su: Department of Biostatistics and Health Data Science, Indiana University School of Medicine, Indianapolis, IN, United States
Qianqian Song: Department of Cancer Biology, Wake Forest School of Medicine, Winston Salem, NC, United States
Qianqian Song: Center for Cancer Genomics and Precision Oncology, Wake Forest School of Medicine, Winston Salem, NC, United States
Michael A. Black: 0Department of Biochemistry, Otago School of Medical Sciences, University of Otago, Dunedin, New Zealand
Cristin Print: 1Department of Molecular Medicine and Pathology and Maurice Wilkins Institute, Faculty of Medical and Health Sciences, The University of Auckland, Auckland, New Zealand
Davide Bedognetti: 2Cancer Program, Sidra Medicine, Doha, Qatar & Department of Internal Medicine and Medical Specialties, University of Genoa, Genoa, Italy
Marissa Howard-McNatt: 3Surgical Oncology Service, Department of Surgery, Wake Forest School of Medicine, Winston Salem, NC, United States
Stacey S. O’Neill: The Comprehensive Cancer Center of Wake Forest University, Winston Salem, NC, United States
Stacey S. O’Neill: 4Department of Pathology, Wake Forest School of Medicine, Winston Salem, NC, United States
Alexandra Thomas: The Comprehensive Cancer Center of Wake Forest University, Winston Salem, NC, United States
Alexandra Thomas: 5Section of Hematology and Oncology, Department of Internal Medicine, Wake Forest Baptist Medical Center, Winston Salem, NC, United States
Carl D. Langefeld: Department of Biostatistics and Data Science, Wake Forest School of Medicine, Winston Salem, NC, United States
Carl D. Langefeld: The Comprehensive Cancer Center of Wake Forest University, Winston Salem, NC, United States
Alexander B. Sigalov: 6 SignaBlok, Inc. Shrewsbury, MA, United States
Yong Lu: The Comprehensive Cancer Center of Wake Forest University, Winston Salem, NC, United States
Yong Lu: 7Department of Microbiology & Immunology, Wake Forest School of Medicine, Winston Salem, NC, United States
Lance D. Miller: Department of Cancer Biology, Wake Forest School of Medicine, Winston Salem, NC, United States
Lance D. Miller: The Comprehensive Cancer Center of Wake Forest University, Winston Salem, NC, United States

DOI: https://doi.org/10.3389/fonc.2021.734959
Journal volume & issue: Vol. 11

Abstract

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BackgroundTriggering receptor expressed on myeloid cells (TREM)-1 is a key mediator of innate immunity previously associated with the severity of inflammatory disorders, and more recently, the inferior survival of lung and liver cancer patients. Here, we investigated the prognostic impact and immunological correlates of TREM1 expression in breast tumors.MethodsBreast tumor microarray and RNAseq expression profiles (n=4,364 tumors) were analyzed for associations between gene expression, tumor immune subtypes, distant metastasis-free survival (DMFS) and clinical response to neoadjuvant chemotherapy (NAC). Single-cell (sc)RNAseq was performed using the 10X Genomics platform. Statistical associations were assessed by logistic regression, Cox regression, Kaplan-Meier analysis, Spearman correlation, Student’s t-test and Chi-square test.ResultsIn pre-treatment biopsies, TREM1 and known TREM-1 inducible cytokines (IL1B, IL8) were discovered by a statistical ranking procedure as top genes for which high expression was associated with reduced response to NAC, but only in the context of immunologically “hot” tumors otherwise associated with a high NAC response rate. In surgical specimens, TREM1 expression varied among tumor molecular subtypes, with highest expression in the more aggressive subtypes (Basal-like, HER2-E). High TREM1 significantly and reproducibly associated with inferior distant metastasis-free survival (DMFS), independent of conventional prognostic markers. Notably, the association between high TREM1 and inferior DMFS was most prominent in the subset of immunogenic tumors that exhibited the immunologically hot phenotype and otherwise associated with superior DMFS. Further observations from bulk and single-cell RNAseq analyses indicated that TREM1 expression was significantly enriched in polymorphonuclear myeloid-derived suppressor cells (PMN-MDSCs) and M2-like macrophages, and correlated with downstream transcriptional targets of TREM-1 (IL8, IL-1B, IL6, MCP-1, SPP1, IL1RN, INHBA) which have been previously associated with pro-tumorigenic and immunosuppressive functions.ConclusionsTogether, these findings indicate that increased TREM1 expression is prognostic of inferior breast cancer outcomes and may contribute to myeloid-mediated breast cancer progression and immune suppression.

Published in Frontiers in Oncology

ISSN: 2234-943X (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://www.frontiersin.org/journals/oncology/

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