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Stem cell CD44v isoforms promote intestinal cancer formation in Apc(min) mice downstream of Wnt signaling.

J Zeilstra ,
S P J Joosten ,
H van Andel ,
C Tolg ,
A Berns ,
M Snoek ,
M van de Wetering ,
M Spaargaren ,
H Clevers ,
S T Pals

Abstract

A gene signature specific for intestinal stem cells (ISCs) has recently been shown to predict relapse in colorectal cancer (CRC) but the tumorigenic role of individual signature genes remains poorly defined. A prominent ISC-signature gene is the cancer stem cell marker CD44, which encodes various splice variants comprising a diverse repertoire of adhesion and signaling molecules. Using Lgr5 as ISC marker, we have fluorescence-activated cell sorting-purified ISCs to define their CD44 repertoire. ISCs display a specific set of CD44 variant isoforms (CD44v), but remarkably lack the CD44 standard (CD44s) isoform. These CD44v also stand-out in transformed human ISCs isolated from microadenomas of familial adenomatous polyposis patients. By employing knock-in mice expressing either CD44v4-10 or CD44s, we demonstrate that the CD44v isoform, but not CD44s, promotes adenoma initiation in Apc(Min/+)mice. Our data identify CD44v as component of the ISCs program critical for tumor initiation, and as potential treatment target in CRC.

More about this publication

Oncogene

Volume 33
Issue nr. 5
Pages 665-70
Publication date 30-01-2014

Full text links

Publisher website (DOI) 10.1038/onc.2012.611
Europe PubMed Central 23318432
Pubmed 23318432

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