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Genomic alterations of the JAK2 and PDL loci occur in a broad spectrum of lymphoid malignancies.

Authors :
UCL - SSS/IREC/MONT - Pôle Mont Godinne
UCL - (MGD) Service d'hématologie
UCL - (MGD) Service d'anatomie pathologique
Van Roosbroeck, Katrien
Ferreiro, Julio Finalet
Tousseyn, Thomas
van der Krogt, Jo-Anne
Michaux, Lucienne
Pienkowska-Grela, Barbara
Théate, Ivan
De Paepe, Pascale
Dierickx, Daan
Doyen, Chantal
Put, Natalie
Cools, Jan
Vandenberghe, Peter
Wlodarska, Iwona
UCL - SSS/IREC/MONT - Pôle Mont Godinne
UCL - (MGD) Service d'hématologie
UCL - (MGD) Service d'anatomie pathologique
Van Roosbroeck, Katrien
Ferreiro, Julio Finalet
Tousseyn, Thomas
van der Krogt, Jo-Anne
Michaux, Lucienne
Pienkowska-Grela, Barbara
Théate, Ivan
De Paepe, Pascale
Dierickx, Daan
Doyen, Chantal
Put, Natalie
Cools, Jan
Vandenberghe, Peter
Wlodarska, Iwona
Source :
Genes, Chromosomes & Cancer, Vol. 55, no. 5, p. 428-441 (2016)
Publication Year :
2016

Abstract

The recurrent 9p24.1 aberrations in lymphoid malignancies potentially involving four cancer-related and druggable genes (JAK2, CD274/PDL1, PDCD1LG2/PDL2, and KDM4C/JMJD2Cl) are incompletely characterized. To gain more insight into the anatomy of these abnormalities, at first we studied 9p24.1 alterations in 18 leukemia/lymphoma cases using cytogenetic and molecular techniques. The aberrations comprised structural (nine cases) and numerical (nine cases) alterations. The former lesions were heterogeneous but shared a common breakpoint region of 200 kb downstream of JAK2. The rearrangements predominantly targeted the PDL locus. We have identified five potential partner genes of PDL1/2: PHACTR4 (1p34), N4BP2 (4p14), EEF1A1 (6q13), JAK2 (9p24.1), and IGL (22q11). Interestingly, the cryptic JAK2-PDL1 rearrangement was generated by a microdeletion spanning the 3'JAK2-5'PDL1 region. JAK2 was additionally involved in a cytogenetically cryptic IGH-mediated t(9;14)(p24.1;q32) found in two patients. This rare but likely underestimated rearrangement highlights the essential role of JAK2 in B-cell neoplasms. Cases with amplification of 9p24.1 were diagnosed as primary mediastinal B-cell lymphoma (five cases) and T-cell lymphoma (four cases). The smallest amplified 9p24.1 region was restricted to the JAK2-PDL1/2-RANBP6 interval. In the next step, we screened 200 cases of classical Hodgkin lymphoma by interphase FISH and identified PDL1/2 rearrangement (CIITA- and IGH-negative) in four cases (2%), what is a novel finding. Forty (25%) cases revealed high level amplification of 9p24.1, including four cases with a selective amplification of PDL1/2. Altogether, the majority of 9p24.1 rearrangements occurring in lymphoid malignancies seem to target the programmed death-1 ligands, what potentiates the therapeutic activity of PD-1 blockade in these tumors. © 2016 Wiley Periodicals, Inc.

Details

Database :
OAIster
Journal :
Genes, Chromosomes & Cancer, Vol. 55, no. 5, p. 428-441 (2016)
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1130470160
Document Type :
Electronic Resource