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Epithelial-to-mesenchymal transition confers pericyte properties on cancer cells

Authors :
Coy D. Heldermon
Yue Jin
Dietmar W. Siemann
Lung-Ji Chang
Christine Pampo
Brian K. Law
Rong Shao
Jianrong Lu
Anitha K. Shenoy
Huacheng Luo
Ming Tang
Lizi Wu
Publication Year :
2016
Publisher :
American Society for Clinical Investigation, 2016.

Abstract

Carcinoma cells can acquire increased motility and invasiveness through epithelial-to-mesenchymal transition (EMT). However, the significance of EMT in cancer metastasis has been controversial, and the exact fates and functions of EMT cancer cells in vivo remain inadequately understood. Here, we tracked epithelial cancer cells that underwent inducible or spontaneous EMT in various tumor transplantation models. Unlike epithelial cells, the majority of EMT cancer cells were specifically located in the perivascular space and closely associated with blood vessels. EMT markedly activated multiple pericyte markers in carcinoma cells, in particular PDGFR-β and N-cadherin, which enabled EMT cells to be chemoattracted towards and physically interact with endothelium. In tumor xenografts generated from carcinoma cells that were prone to spontaneous EMT, a substantial fraction of the pericytes associated with tumor vasculature were derived from EMT cancer cells. Depletion of such EMT cells in transplanted tumors diminished pericyte coverage, impaired vascular integrity, and attenuated tumor growth. These findings suggest that EMT confers key pericyte attributes on cancer cells. The resulting EMT cells phenotypically and functionally resemble pericytes and are indispensable for vascular stabilization and sustained tumor growth. This study thus proposes a previously unrecognized role for EMT in cancer.

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....c0da60220752f0565788d9b0cc6c50cc