TY - JOUR
T1 - Single-cell analysis reveals a stem-cell program in human metastatic breast cancer cells
AU - Lawson, Devon A.
AU - Bhakta, Nirav R.
AU - Kessenbrock, Kai
AU - Prummel, Karin D.
AU - Yu, Ying
AU - Takai, Ken
AU - Zhou, Alicia
AU - Eyob, Henok
AU - Balakrishnan, Sanjeev
AU - Wang, Chih Yang
AU - Yaswen, Paul
AU - Goga, Andrei
AU - Werb, Zena
N1 - Funding Information:
Acknowledgements We thank A. Welm for providing access to PDX tissues developed by her group, which served as the foundation for this study. We also thank K. Lee, R. Kumar, A. Le, R. Daneman, J. Stingl and M. Binneweis for comments and technical contributions. This study was supported by funds from the National Cancer Institute (CA180039 and CA136717), Stand Up To Cancer/AACR (DT0409), the Era of Hope Scholar Award (W81XWH-12-1-0272), the Breast Cancer Research Foundation and the Atwater Foundation, and D. and J. Vander Wall. D.A.L. was supported by a US Department of Defense Congressionally Directed Medical Research Program postdoctoral fellowship (11-1-0742), and C.W. is supported by a grant from the Ministry of Science and Technology, Taiwan (104-2917-I-006-002).
Publisher Copyright:
© 2015 Macmillan Publishers Limited. All rights reserved.
PY - 2015/10/1
Y1 - 2015/10/1
N2 - Despite major advances in understanding the molecular and genetic basis of cancer, metastasis remains the cause of >90% of cancer-related mortality. Understanding metastasis initiation and progression is critical to developing new therapeutic strategies to treat and prevent metastatic disease. Prevailing theories hypothesize that metastases are seeded by rare tumour cells with unique properties, which may function like stem cells in their ability to initiate and propagate metastatic tumours. However, the identity of metastasis-initiating cells in human breast cancer remains elusive, and whether metastases are hierarchically organized is unknown. Here we show at the single-cell level that early stage metastatic cells possess a distinct stem-like gene expression signature. To identify and isolate metastatic cells from patient-derived xenograft models of human breast cancer, we developed a highly sensitive fluorescence-activated cell sorting (FACS)-based assay, which allowed us to enumerate metastatic cells in mouse peripheral tissues. We compared gene signatures in metastatic cells from tissues with low versus high metastatic burden. Metastatic cells from low-burden tissues were distinct owing to their increased expression of stem cell, epithelial-to-mesenchymal transition, pro-survival, and dormancy-associated genes. By contrast, metastatic cells from high-burden tissues were similar to primary tumour cells, which were more heterogeneous and expressed higher levels of luminal differentiation genes. Transplantation of stem-like metastatic cells from low-burden tissues showed that they have considerable tumour-initiating capacity, and can differentiate to produce luminal-like cancer cells. Progression to high metastatic burden was associated with increased proliferation and MYC expression, which could be attenuated by treatment with cyclin-dependent kinase (CDK) inhibitors. These findings support a hierarchical model for metastasis, in which metastases are initiated by stem-like cells that proliferate and differentiate to produce advanced metastatic disease.
AB - Despite major advances in understanding the molecular and genetic basis of cancer, metastasis remains the cause of >90% of cancer-related mortality. Understanding metastasis initiation and progression is critical to developing new therapeutic strategies to treat and prevent metastatic disease. Prevailing theories hypothesize that metastases are seeded by rare tumour cells with unique properties, which may function like stem cells in their ability to initiate and propagate metastatic tumours. However, the identity of metastasis-initiating cells in human breast cancer remains elusive, and whether metastases are hierarchically organized is unknown. Here we show at the single-cell level that early stage metastatic cells possess a distinct stem-like gene expression signature. To identify and isolate metastatic cells from patient-derived xenograft models of human breast cancer, we developed a highly sensitive fluorescence-activated cell sorting (FACS)-based assay, which allowed us to enumerate metastatic cells in mouse peripheral tissues. We compared gene signatures in metastatic cells from tissues with low versus high metastatic burden. Metastatic cells from low-burden tissues were distinct owing to their increased expression of stem cell, epithelial-to-mesenchymal transition, pro-survival, and dormancy-associated genes. By contrast, metastatic cells from high-burden tissues were similar to primary tumour cells, which were more heterogeneous and expressed higher levels of luminal differentiation genes. Transplantation of stem-like metastatic cells from low-burden tissues showed that they have considerable tumour-initiating capacity, and can differentiate to produce luminal-like cancer cells. Progression to high metastatic burden was associated with increased proliferation and MYC expression, which could be attenuated by treatment with cyclin-dependent kinase (CDK) inhibitors. These findings support a hierarchical model for metastasis, in which metastases are initiated by stem-like cells that proliferate and differentiate to produce advanced metastatic disease.
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U2 - 10.1038/nature15260
DO - 10.1038/nature15260
M3 - Article
C2 - 26416748
AN - SCOPUS:84943143136
SN - 0028-0836
VL - 526
SP - 131
EP - 135
JO - Nature
JF - Nature
IS - 7571
ER -
