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Circulating Tumor Cell Clusters Are Oligoclonal Precursors of Breast Cancer Metastasis

Overview
Journal Cell
Publisher Cell Press
Specialty Cell Biology
Date 2014 Aug 30
PMID 25171411
Citations 1245
Authors
Nicola Aceto
Aditya Bardia
David T Miyamoto
Maria C Donaldson
Ben S Wittner
Joel A Spencer
Min Yu
Adam Pely
Amanda Engstrom
Huili Zhu
Brian W Brannigan
Ravi Kapur
Shannon L Stott
Toshi Shioda
Sridhar Ramaswamy
David T Ting
Charles P Lin
Mehmet Toner
Daniel A Haber
Shyamala Maheswaran
Affiliations
Soon will be listed here.
Abstract

Circulating tumor cell clusters (CTC clusters) are present in the blood of patients with cancer but their contribution to metastasis is not well defined. Using mouse models with tagged mammary tumors, we demonstrate that CTC clusters arise from oligoclonal tumor cell groupings and not from intravascular aggregation events. Although rare in the circulation compared with single CTCs, CTC clusters have 23- to 50-fold increased metastatic potential. In patients with breast cancer, single-cell resolution RNA sequencing of CTC clusters and single CTCs, matched within individual blood samples, identifies the cell junction component plakoglobin as highly differentially expressed. In mouse models, knockdown of plakoglobin abrogates CTC cluster formation and suppresses lung metastases. In breast cancer patients, both abundance of CTC clusters and high tumor plakoglobin levels denote adverse outcomes. Thus, CTC clusters are derived from multicellular groupings of primary tumor cells held together through plakoglobin-dependent intercellular adhesion, and though rare, they greatly contribute to the metastatic spread of cancer.

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