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Mice deficient for CD137 ligand are predisposed to develop germinal center-derived B-cell lymphoma.

Sabine Middendorp ,
Yanling Xiao ,
Ji-Ying Song ,
Victor Peperzak ,
Peter H L Krijger ,
Heinz Jacobs ,
Jannie Borst

Abstract

In the germinal center (GC), B cells proliferate dramatically and diversify their immunoglobulin genes, which increases the risk of malignant transformation. The GC B-cell reaction relies on crosstalk with follicular dendritic cells (FDCs), to which the costimulatory receptor CD137 on FDCs and its ligand on GC B cells potentially contribute. We report that mice deficient for CD137 ligand (CD137L) are predisposed to develop B-cell lymphoma, with an incidence of approximately 60% at 12 months of age. Lymphoma membrane markers were characteristic of GC B cells. Longitudinal histologic analysis identified the GC as site of oncogenic transformation and classified 85% of the malignancies found in approximately 200 mice as GC-derived B-cell lymphoma. To delineate the mechanism underlying lymphomagenesis, gene expression profiles of wild-type and CD137L-deficient GC B cells were compared. CD137L deficiency was associated with enhanced expression of a limited gene set that included Bcl-10 and the GC response regulators Bcl-6, Spi-B, Elf-1, Bach2, and activation-induced cytidine deaminase. Among these are proto-oncogenes that mediate GC B-cell lymphoma development in humans. We conclude that CD137L ordinarily regulates the GC B-cell response and thereby acts as a tumor suppressor.

More about this publication

Blood

Volume 114
Issue nr. 11
Pages 2280-9
Publication date 10-09-2009

Full text links

Publisher website (DOI) 10.1182/blood-2009-03-208215
Europe PubMed Central 19608748
Pubmed 19608748

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