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TET2 controls chemoresistant slow-cycling cancer cell survival and tumor recurrence

Authors :
Puig, Isabel
Tenbaum, Stephan P.
Chicote, Irene
Arques, Oriol
Martinez- Quintanilla, Jordi
Cuesta-Borras, Estefania
Ramirez, Lorena
Gonzalo, Pilar
Soto, Atenea
Aguilar, Susana
Eguizabal, Cristina
Caratu, Ginevra
Prat, Aleix
Argiles, Guillem
Landolfi, Stefania
Casanovas, Oriol
Serra, Violeta
Villanueva, Alberto
Arroyo, Alicia G.
Terracciano, Luigi
Nuciforo, Paolo
Seoane, Joan
Recio, Juan A.
Vivancos, Ana
Dienstmann, Rodrigo
Tabernero, Josep
Palmer, Hector G.
Source :
Journal of Clinical Investigation. September 2018, Vol. 128 Issue 9, p3887, 19 p.
Publication Year :
2018

Abstract

Introduction Cancer remains a deadly disease since patients often relapse after surgery and adjuvant therapy, progressing to advanced metastatic stages (1). Recent studies have shown that cancer cells, beyond their [...]<br />Dormant or slow-cycling tumor cells can form a residual chemoresistant reservoir responsible for relapse in patients, years after curative surgery and adjuvant therapy. We have adapted the pulse-chase expression of H2BeGFP for labeling and isolating slow-cycling cancer cells (SCCCs). SCCCs showed cancer initiation potential and enhanced chemoresistance. Cells at this slow-cycling status presented a distinctive nongenetic and cell- autonomous gene expression profile shared across different tumor types. We identified TET2 epigenetic enzyme as a key factor controlling SCCC numbers, survival, and tumor recurrence. 5-Hydroxymethylcytosine (5hmC), generated by TET2 enzymatic activity, labeled the SCCC genome in carcinomas and was a predictive biomarker of relapse and survival in cancer patients. We have shown the enhanced chemoresistance of SCCCs and revealed 5hmC as a biomarker for their clinical identification and TET2 as a potential drug target for SCCC elimination that could extend patients' survival.

Details

Language :
English
ISSN :
00219738
Volume :
128
Issue :
9
Database :
Gale General OneFile
Journal :
Journal of Clinical Investigation
Publication Type :
Academic Journal
Accession number :
edsgcl.553759913
Full Text :
https://doi.org/10.1172/JCI96393