Gene expression profiling identifies emerging oncogenic pathways operating in extranodal NK/T-cell lymphoma, nasal type.

Gaulard, P.

doi:10.1182/blood-2009-05-221275

Titre

Gene expression profiling identifies emerging oncogenic pathways operating in extranodal NK/T-cell lymphoma, nasal type.

Type

article

Institution

Externe

Périodique

Blood

Auteur(s)

Huang, Y.

Auteure/Auteur

de Reyniès, A.

Auteure/Auteur

de Leval, L.

Auteure/Auteur

Ghazi, B.

Auteure/Auteur

Martin-Garcia, N.

Auteure/Auteur

Travert, M.

Auteure/Auteur

Bosq, J.

Auteure/Auteur

Brière, J.

Auteure/Auteur

Petit, B.

Auteure/Auteur

Thomas, E.

Auteure/Auteur

Coppo, P.

Auteure/Auteur

Marafioti, T.

Auteure/Auteur

Emile, J.F.

Auteure/Auteur

Delfau-Larue, M.H.

Auteure/Auteur

Schmitt, C.

Auteure/Auteur

Gaulard, P.

Auteure/Auteur

Liens vers les personnes

de Leval, Laurence

ISSN

1528-0020[electronic], 0006-4971[linking]

Statut éditorial

Publié

Date de publication

2010

Volume

115

Numéro

6

Première page

1226

Dernière page/numéro d’article

1237

Langue

anglais

Résumé

Biopsies and cell lines of natural killer/T-cell lymphoma, nasal type (NKTCL) were subject to combined gene expression profiling and array-based comparative genomic hybridization analyses. Compared with peripheral T-cell lymphoma, not otherwise specified, NKTCL had greater transcript levels for NK-cell and cytotoxic molecules, especially granzyme H. Compared with normal NKcells, tumors were closer to activated than resting cells and overexpressed several genes related to vascular biology, Epstein-Barr Virus-induced genes, and PDGFRA. Notably, platelet-derived growth factor receptor alpha and its phosphorylated form were confirmed at the protein level, and in vitro the MEC04 NKTCL cell line was sensitive to imatinib. Deregulation of the AKT, Janus kinase-signal transducers and activators of transcription, and nuclear factor-kappaB pathways was corroborated by nuclear expression of phosphorylated AKT, signal transducers and activators of transcription 3, and RelA in NKTCL, and several deregulated genes in these pathways mapped to regions of recurrent copy number aberrations (AKT3 [1q44], IL6R [1q21.3], CCL2 [17q12], TNFRSF21 [6p12.3]). Several features of NKTCL uncovered by this analysis suggest perturbation of angiogenic pathways. Integrative analysis also evidenced deregulation of the tumor suppressor HACE1 in the frequently deleted 6q21 region. This study highlights emerging oncogenic pathways in NKTCL and identifies novel diagnostic and therapeutic targets.

PID Serval

serval:BIB_17A96CCBC0E5

DOI

10.1182/blood-2009-05-221275

PMID

19965620

Permalien

https://iris.unil.ch/handle/iris/31697

Open Access

Oui

Date de création

2010-10-22T08:51:32.339Z

Date de création dans IRIS

2025-05-20T13:19:58Z