Single-Cell Map of Diverse Immune Phenotypes in the Breast Tumor Microenvironment
Author(s) -
Elham Azizi,
Ambrose Carr,
George Plitas,
Andrew Cornish,
Catherine Konopacki,
Sandhya Prabhakaran,
Juozas Nainys,
Kenmin Wu,
Vaidotas Kiseliovas,
Manu Setty,
Kristy Choi,
Rachel M. Fromme,
Phuong Dao,
Peter T. McKenney,
Ruby Wasti,
Krishna Kadaveru,
Linas Mažutis,
Alexander Y. Rudensky,
Dana Pe’er
Publication year - 2018
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2018.05.060
Subject(s) - biology , tumor microenvironment , immune system , t cell receptor , phenotype , t cell , cancer immunology , single cell analysis , single cell sequencing , cell , breast cancer , cancer research , immunotherapy , immunology , cancer , computational biology , gene , genetics , exome sequencing
Knowledge of immune cell phenotypes in the tumor microenvironment is essential for understanding mechanisms of cancer progression and immunotherapy response. We profiled 45,000 immune cells from eight breast carcinomas, as well as matched normal breast tissue, blood, and lymph nodes, using single-cell RNA-seq. We developed a preprocessing pipeline, SEQC, and a Bayesian clustering and normalization method, Biscuit, to address computational challenges inherent to single-cell data. Despite significant similarity between normal and tumor tissue-resident immune cells, we observed continuous phenotypic expansions specific to the tumor microenvironment. Analysis of paired single-cell RNA and T cell receptor (TCR) sequencing data from 27,000 additional T cells revealed the combinatorial impact of TCR utilization on phenotypic diversity. Our results support a model of continuous activation in T cells and do not comport with the macrophage polarization model in cancer. Our results have important implications for characterizing tumor-infiltrating immune cells.
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