A Novel Platform for Detection of CK+ and CK- CTCs

Overview

Journal Cancer Discov

Specialty Oncology

Date 2011 Dec 20

PMID 22180853

Citations 98

Authors

Chad V Pecot

Farideh Z Bischoff

Julie Ann Mayer

Karina L Wong

Tam Pham

Justin Bottsford-Miller

Rebecca L Stone

Yvonne G Lin

Padmavathi Jaladurgam

Ju Won Roh

Blake W Goodman

William M Merritt

Tony J Pircher

Stephen D Mikolajczyk

Alpa M Nick

Joseph Celestino

Cathy Eng

Lee M Ellis

Michael T Deavers

Anil K Sood

Affiliations

Soon will be listed here.

Abstract

Unlabelled: Metastasis is a complex, multistep process that begins with the epithelial-mesenchymal transition (EMT). Circulating tumor cells (CTC) are believed to have undergone EMT and thus lack or express low levels of epithelial markers commonly used for enrichment and/or detection of such cells. However, most current CTC detection methods target only EpCAM and/or cytokeratin (CK) to enrich epithelial CTCs, resulting in failure to recognize other, perhaps more important, CTC phenotypes that lack expression of these markers. Here, we describe a population of complex aneuploid CTCs that do not express CK or CD45 antigen in patients with breast, ovarian, or colorectal cancer. These cells were not observed in healthy subjects. We show that the primary epithelial tumors were characterized by similar complex aneuploidy, indicating conversion to an EMT phenotype in the captured cells. Collectively, our study provides a new method for highly efficient capture of previously unrecognized populations of CTCs.

Significance: Current assays for CTC capture likely miss populations of cells that have undergone EMT. Capture and study of CTCs that have undergone EMT would allow a better understanding of the mechanisms driving metastasis.

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