Unravelling Subclonal Heterogeneity and Aggressive Disease States in TNBC Through Single-cell RNA-seq

Overview

Journal Nat Commun

Specialty Biology

Date 2018 Sep 6

PMID 30181541

Citations 247

Authors

Mihriban Karaayvaz

Simona Cristea

Shawn M Gillespie

Anoop P Patel

Ravindra Mylvaganam

Christina C Luo

Michelle C Specht

Bradley E Bernstein

Franziska Michor

Leif W Ellisen

Affiliations

Soon will be listed here.

Abstract

Triple-negative breast cancer (TNBC) is an aggressive subtype characterized by extensive intratumoral heterogeneity. To investigate the underlying biology, we conducted single-cell RNA-sequencing (scRNA-seq) of >1500 cells from six primary TNBC. Here, we show that intercellular heterogeneity of gene expression programs within each tumor is variable and largely correlates with clonality of inferred genomic copy number changes, suggesting that genotype drives the gene expression phenotype of individual subpopulations. Clustering of gene expression profiles identified distinct subgroups of malignant cells shared by multiple tumors, including a single subpopulation associated with multiple signatures of treatment resistance and metastasis, and characterized functionally by activation of glycosphingolipid metabolism and associated innate immunity pathways. A novel signature defining this subpopulation predicts long-term outcomes for TNBC patients in a large cohort. Collectively, this analysis reveals the functional heterogeneity and its association with genomic evolution in TNBC, and uncovers unanticipated biological principles dictating poor outcomes in this disease.

Citing Articles

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