| Literature DB >> 33950524 |
Bhupinder Pal1,2,3,4, Yunshun Chen2,5, François Vaillant1,2, Bianca D Capaldo1,2, Rachel Joyce1,2, Xiaoyu Song1,2, Vanessa L Bryant2,6, Jocelyn S Penington2,5, Leon Di Stefano2,5, Nina Tubau Ribera7,8, Stephen Wilcox8, Gregory B Mann9,10,11,12, Anthony T Papenfuss2,5, Geoffrey J Lindeman1,9,10,13, Gordon K Smyth5,14, Jane E Visvader1,2.
Abstract
To examine global changes in breast heterogeneity across different states, we determined the single-cell transcriptomes of > 340,000 cells encompassing normal breast, preneoplastic BRCA1+/- tissue, the major breast cancer subtypes, and pairs of tumors and involved lymph nodes. Elucidation of the normal breast microenvironment revealed striking changes in the stroma of post-menopausal women. Single-cell profiling of 34 treatment-naive primary tumors, including estrogen receptor (ER)+ , HER2+ , and triple-negative breast cancers, revealed comparable diversity among cancer cells and a discrete subset of cycling cells. The transcriptomes of preneoplastic BRCA1+/- tissue versus tumors highlighted global changes in the immune microenvironment. Within the tumor immune landscape, proliferative CD8+ T cells characterized triple-negative and HER2+ cancers but not ER+ tumors, while all subtypes comprised cycling tumor-associated macrophages, thus invoking potentially different immunotherapy targets. Copy number analysis of paired ER+ tumors and lymph nodes indicated seeding by genetically distinct clones or mass migration of primary tumor cells into axillary lymph nodes. This large-scale integration of patient samples provides a high-resolution map of cell diversity in normal and cancerous human breast.Entities:
Keywords: BRCA1 carriers; LN metastasis; breast cancer; microenvironment; single-cell RNA-seq
Year: 2021 PMID: 33950524 DOI: 10.15252/embj.2020107333
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 11.598