Mantle cell lymphoma-like lymphomas in c-myc-3’RR/p53+/- mice and c-myc-3’RR/Cdk4R24C mice: differential oncogenic mechanisms but similar cellular origin

Pauline Rouaud; Rémi Fiancette; Christelle Vincent-Fabert; Virginie Magnone; Michel Cogné; Pierre Dubus; Yves Denizot

doi:10.18632/oncotarget.474

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Methodological Reports:

Mantle cell lymphoma-like lymphomas in c-myc-3’RR/p53+/- mice and c-myc-3’RR/Cdk4R24C mice: differential oncogenic mechanisms but similar cellular origin

Pauline Rouaud, Rémi Fiancette, Christelle Vincent-Fabert, Virginie Magnone, Michel Cogné, Pierre Dubus and Yves Denizot _

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Oncotarget. 2012; 3:586-593. https://doi.org/10.18632/oncotarget.474

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Abstract

Pauline Rouaud¹, Rémi Fiancette¹, Christelle Vincent-Fabert¹, Virginie Magnone², Michel Cogné¹, Pierre Dubus³ and Yves Denizot¹

¹ UMR CNRS 7276, Faculté de Médecine, Limoges, France

² CNRS and University of Nice Sophia Antipolis, Institut de Pharmacologie Moléculaire et Cellulaire, UMR 6097, Sophia Antipolis, France

³ EA2406, Université de Bordeaux, Bordeaux, France

Received: April 3, 2012; Accepted: April 28, 2012; Published: May 9, 2012;

Keywords: Mantle cell lymphoma, c-myc

Correspondence:

Yves Denizot, email:

Abstract

Mantle cell lymphoma (MCL) is a malignant lymphoproliferative B-cell disorder that does not occur spontaneously in mice but experimental mice model have been developed. Recently two different mice models prone to develop MCL-like lymphomas were generated: c-myc-3’RR/Cdk4^R24C mice and c-myc-3’RR/p53^+/- mice. Comparison of their gene expression profiles does not highlight specific differences other than those in relation with their specific mutational status (i.e., Cdk4^R24C mutation or p53 mutation). We propose that similarly to typical human MCL and its blastoid or cyclin-D1 variants that correspond to the same genetic entity, MCL-like lymphomas of c-myc-3’RR/p53^+/- mice and c-myc-3’RR/Cdk4^R24C mice represent a spectrum of the same entity.

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Methodological Reports:

Mantle cell lymphoma-like lymphomas in c-myc-3’RR/p53+/- mice and c-myc-3’RR/Cdk4R24C mice: differential oncogenic mechanisms but similar cellular origin

Abstract