TY - JOUR
T1 - Polyclonal breast cancer metastases arise from collective dissemination of keratin 14-expressing tumor cell clusters
AU - Cheung, Kevin J.
AU - Padmanaban, Veena
AU - Silvestri, Vanesa
AU - Schipper, Koen
AU - Cohen, Joshua D.
AU - Fairchild, Amanda N.
AU - Gorin, Michael A.
AU - Verdone, James E.
AU - Pienta, Kenneth J.
AU - Bader, Joel S.
AU - Ewald, Andrew J.
N1 - Funding Information:
We thank members of the A.J.E. laboratory for comments on the manuscript; B. Stanger and R. Maddipati for sharing unpublished data; Hao Zhang of The Johns Hopkins School of Public Health Flow Cytometry Core Facility for assistance with FACS; and Haiping Hao of The Johns Hopkins Medical Institutions Deep Sequencing and Microarray Core Facility for assistance with RNA-seq. K.J.C. is supported by a Postdoctoral Fellowship from the US Department of Defense (W81XWH-12-1-0018) and a Burroughs Wellcome Fund Career Award for Medical Scientists. A.J.E. is supported by a Research Scholar Grant (RSG-12-141-01-CSM) from the American Cancer Society, by funds from the National Institutes of Health/National Cancer Institute (P30 CA006973), by a grant from the Mary Kay Ash Foundation (036-13), by funds from the Cindy Rosencrans Fund for Triple Negative Breast Cancer Research, by a Research Leadership Award from the Metastatic Breast Cancer Network, and by an award from The Pink Agenda and The Breast Cancer Research Foundation.
PY - 2016/2/16
Y1 - 2016/2/16
N2 - Recent genomic studies challenge the conventional model that each metastasis must arise from a single tumor cell and instead reveal that metastases can be composed of multiple genetically distinct clones. These intriguing observations raise the question: How do polyclonal metastases emerge from the primary tumor? In this study, we used multicolor lineage tracing to demonstrate that polyclonal seeding by cell clusters is a frequent mechanism in a common mouse model of breast cancer, accounting for >90% of metastases. We directly observed multicolored tumor cell clusters across major stages of metastasis, including collective invasion, local dissemination, intravascular emboli, circulating tumor cell clusters, and micrometastases. Experimentally aggregating tumor cells into clusters induced a >15-fold increase in colony formation ex vivo and a >100-fold increase in metastasis formation in vivo. Intriguingly, locally disseminated clusters, circulating tumor cell clusters, and lung micrometastases frequently expressed the epithelial cytoskeletal protein, keratin 14 (K14). RNA-seq analysis revealed that K14+ cells were enriched for desmosome and hemidesmosome adhesion complex genes, and were depleted for MHC class II genes. Depletion of K14 expression abrogated distant metastases and disrupted expression of multiple metastasis effectors, including Tenascin C (Tnc), Jagged1 (Jag1), and Epiregulin (Ereg). Taken together, our findings reveal K14 as a key regulator of metastasis and establish the concept that K14+ epithelial tumor cell clusters disseminate collectively to colonize distant organs.
AB - Recent genomic studies challenge the conventional model that each metastasis must arise from a single tumor cell and instead reveal that metastases can be composed of multiple genetically distinct clones. These intriguing observations raise the question: How do polyclonal metastases emerge from the primary tumor? In this study, we used multicolor lineage tracing to demonstrate that polyclonal seeding by cell clusters is a frequent mechanism in a common mouse model of breast cancer, accounting for >90% of metastases. We directly observed multicolored tumor cell clusters across major stages of metastasis, including collective invasion, local dissemination, intravascular emboli, circulating tumor cell clusters, and micrometastases. Experimentally aggregating tumor cells into clusters induced a >15-fold increase in colony formation ex vivo and a >100-fold increase in metastasis formation in vivo. Intriguingly, locally disseminated clusters, circulating tumor cell clusters, and lung micrometastases frequently expressed the epithelial cytoskeletal protein, keratin 14 (K14). RNA-seq analysis revealed that K14+ cells were enriched for desmosome and hemidesmosome adhesion complex genes, and were depleted for MHC class II genes. Depletion of K14 expression abrogated distant metastases and disrupted expression of multiple metastasis effectors, including Tenascin C (Tnc), Jagged1 (Jag1), and Epiregulin (Ereg). Taken together, our findings reveal K14 as a key regulator of metastasis and establish the concept that K14+ epithelial tumor cell clusters disseminate collectively to colonize distant organs.
KW - Breast cancer
KW - Collective dissemination
KW - Collective invasion
KW - Keratin 14
KW - Polyclonal metastasis
UR - http://www.scopus.com/inward/record.url?scp=84958818284&partnerID=8YFLogxK
U2 - 10.1073/pnas.1508541113
DO - 10.1073/pnas.1508541113
M3 - Article
C2 - 26831077
AN - SCOPUS:84958818284
SN - 0027-8424
VL - 113
SP - E854-E863
JO - Proceedings of the National Academy of Sciences of the United States of America
JF - Proceedings of the National Academy of Sciences of the United States of America
IS - 7
ER -