Single-cell evaluation reveals shifts in the tumor-immune niches that shape and maintain aggressive lesions in the breast

Author:

Sinha Vidya C.ORCID,Rinkenbaugh Amanda L.,Xu Mingchu,Zhou Xinhui,Zhang XiaomeiORCID,Jeter-Jones Sabrina,Shao Jiansu,Qi YuanORCID,Zebala John A.,Maeda Dean Y.ORCID,McAllister FlorenciaORCID,Piwnica-Worms HelenORCID

Abstract

AbstractThere is an unmet clinical need for stratification of breast lesions as indolent or aggressive to tailor treatment. Here, single-cell transcriptomics and multiparametric imaging applied to a mouse model of breast cancer reveals that the aggressive tumor niche is characterized by an expanded basal-like population, specialization of tumor subpopulations, and mixed-lineage tumor cells potentially serving as a transition state between luminal and basal phenotypes. Despite vast tumor cell-intrinsic differences, aggressive and indolent tumor cells are functionally indistinguishable once isolated from their local niche, suggesting a role for non-tumor collaborators in determining aggressiveness. Aggressive lesions harbor fewer total but more suppressed-like T cells, and elevated tumor-promoting neutrophils and IL-17 signaling, disruption of which increase tumor latency and reduce the number of aggressive lesions. Our study provides insight into tumor-immune features distinguishing indolent from aggressive lesions, identifies heterogeneous populations comprising these lesions, and supports a role for IL-17 signaling in aggressive progression.

Funder

U.S. Department of Health & Human Services | National Institutes of Health

U.S. Department of Defense

Cancer Prevention and Research Institute of Texas

EIF | Stand Up To Cancer

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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