Loss of p73 promotes dissemination of Myc-induced B cell lymphomas in mice
Alice Nemajerova, … , Gustavo Palacios, Ute M. Moll
Alice Nemajerova, … , Gustavo Palacios, Ute M. Moll
Published May 17, 2010
Citation Information: J Clin Invest. 2010;120(6):2070-2080. https://doi.org/10.1172/JCI40331.
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Research Article Hematology

Loss of p73 promotes dissemination of Myc-induced B cell lymphomas in mice

Abstract

Mice engineered to express c-Myc in B cells (Eμ-myc mice) develop lethal lymphomas in which the gene encoding the p53 tumor suppressor is frequently mutated. Whether the p53 homolog p73 also functions as a tumor suppressor in vivo remains controversial. Here we have shown that p73 loss does not substantially affect disease onset and mortality in Eμ-myc mice. However, it does alter the phenotype of the disease. Specifically, p73 loss decreased nodal disease and increased widespread extranodal dissemination. We further found that p53 acted as the dominant tumor suppressor during the onset of Eμ-myc–driven B cell lymphomagenesis, while p73 modulated tumor dissemination and extranodal growth. Immunophenotyping and expression profiling suggested that p73 loss allowed increased maturation of malignant B cells and deregulated genes involved in lymphocyte homing and dissemination of human lymphomas. Consistent with this, p73 expression was frequently downregulated in a large cohort of human mature aggressive B cell lymphomas, and both the incidence and degree of p73 downregulation in these tumors correlated with their extranodal dissemination status. These data indicate that p73 is a modifier of Myc-driven lymphomas in mice, favoring tumor dissemination, and suggest that p73 could be a biomarker for human B cell lymphoma dissemination, a notion that can now be tested in clinicopathologic correlation studies.

Authors

Alice Nemajerova, Oleksi Petrenko, Lorenz Trümper, Gustavo Palacios, Ute M. Moll

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Figure 4

Loss of p73 promotes dissemination of Eμ-myc lymphomas.

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Loss of p73 promotes dissemination of Eμ-myc lymphomas. (A) Representati...
(A) Representative moribund p73+/+Eμ-myc and p73–/– Eμ-myc mice are shown. Arrows, spleens; circles, lymph nodes. For comparison, spleens have been placed on top of the bowel. (B) Average weight of spleen and lymph nodes (compound per animal) from moribund Eμ-myc p73+/+, p73+/–, and p73–/– mice. Error bars represent SEM derived from 20 mice of each genotype. (C) Histological examination (H&E staining) of lymphoma dissemination in p73–/– Eμ-myc mice. Arrows denote lymphomatous infiltrates in lung and brain parenchyma. Original magnification, ×4 (left); ×10 (right). (D) Weight of reconstituted lymphomas in nude mice inoculated with Eμ-myc p73+/+ and p73–/– lymphoma cells (1 × 106 cells each). Error bars represent SEM from 4 independent experiments. (E) Immunophenotyping of tumors from p73+/+ and p73–/– Eμ-myc mice with B220, CD19, and IgM antibodies. Tumors were classified as either predominantly (>80%) IgM-positive (mature) or IgM-negative (immature). (F) Quantitative real-time RT-PCR analysis of AID in Eμ-myc p73+/+ and p73–/– lymphomas (7 random tumors per genotype).