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A Single-Cell Immune Atlas of Triple Negative Breast Cancer Reveals Novel Immune Cell Subsets

Authors :
Qiu, Si
Hong, Ruoxi
Zhuang, Zhenkun
Li, Yuan
Zhu, Linnan
Lin, Xinxin
Zheng, Qiufan
Liu, Shang
Zhang, Kai
Huang, Mengxian
Lee, Kaping
Lu, Qianyi
Xia, Wen
Xu, Fei
Wang, Xi
Tang, Jun
Xiao, Xiangsheng
Wei, Weidong
Yuan, Zhongyu
Shi, Yanxia
Hou, Yong
Zhang, Xiuqing
Wang, Jian
Yang, Huanming
Zhan, Qimin
Li, Bo
Wang, Shusen
Publication Year :
2019
Publisher :
Cold Spring Harbor Laboratory, 2019.

Abstract

Triple-negative breast cancer (TNBC) represents the most aggressive breast cancer subtype, which recently attracts great interest for immune therapeutic development. In this context, in-depth understanding of TNBC immune landscape is highly demanded. Here we report single-cell RNA sequencing results of 9683 tumor-infiltrated immune cells isolated from 14 treatment naïve TNBC tumors, where 22 immune cell subsets, including T cells, macrophages, B cells, and DCs have been characterized. We identify a new T cell subset, CD8+CXCL8+ naïve T cell, which associates with poor survival. A novel immune cell subset comprised of TCR+ macrophages, is found to be widely distributed in TNBC tumors. Further analyses reveal an up-regulation of molecules associated with TCR signaling and cytotoxicity in these immune cells, indicating TCR signaling activation. Altogether, our study provides a valuable resource to understand the immune ecosystem of TNBC. The novel immune cell subsets reported herein might be functionally important in cancer immunity.SIGNIFICANCEThis work demonstrates a single-cell transcriptome atlas of immune cells in treatment naïve TNBC tumors, revealing novel immune cell subsets. This study provides a valuable resource to understand the immune ecosystem of TNBC, which will be helpful for the immunotherapeutic strategy design of TNBC.

Details

Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....fd27dab9f1d671f618c7d19704451fdd