MDM4 Is Targeted by 1q Gain and Drives Disease in Burkitt Lymphoma

Overview

Journal Cancer Res

Specialty Oncology

Date 2019 Apr 20

PMID 31000522

Citations 18

Authors

Jennifer Hullein

Mikolaj Slabicki

Maciej Rosolowski

Alexander Jethwa

Stefan Habringer

Katarzyna Tomska

Roma Kurilov

Junyan Lu

Sebastian Scheinost

Rabea Wagener

Zhiqin Huang

Marina Lukas

Olena Yavorska

Hanne Helfrich

Rene Scholtysik

Kyle Bonneau

Donato Tedesco

Ralf Kuppers

Wolfram Klapper

Christiane Pott

Stephan Stilgenbauer

Birgit Burkhardt

Markus Loffler

Lorenz H Trumper

Michael Hummel

Benedikt Brors

Marc Zapatka

Reiner Siebert

Markus Kreuz

Ulrich Keller

Wolfgang Huber

Thorsten Zenz

Affiliations

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Abstract

Oncogenic MYC activation promotes proliferation in Burkitt lymphoma, but also induces cell-cycle arrest and apoptosis mediated by p53, a tumor suppressor that is mutated in 40% of Burkitt lymphoma cases. To identify molecular dependencies in Burkitt lymphoma, we performed RNAi-based, loss-of-function screening in eight Burkitt lymphoma cell lines and integrated non-Burkitt lymphoma RNAi screens and genetic data. We identified 76 genes essential to Burkitt lymphoma, including genes associated with hematopoietic cell differentiation () or B-cell development and activation () and found a number of context-specific dependencies including oncogene addiction in cell lines with / or mutation. The strongest genotype-phenotype association was seen for . MDM4, a negative regulator of , was essential in wild-type (TP53wt) Burkitt lymphoma cell lines. knockdown activated p53, induced cell-cycle arrest, and decreased tumor growth in a xenograft model in a p53-dependent manner. Small molecule inhibition of the MDM4-p53 interaction was effective only in TP53wt Burkitt lymphoma cell lines. Moreover, primary TP53wt Burkitt lymphoma samples frequently acquired gains of chromosome 1q, which includes the locus, and showed elevated MDM4 mRNA levels. 1q gain was associated with TP53wt across 789 cancer cell lines and was essential in the TP53wt-context in 216 cell lines representing 19 cancer entities from the Achilles Project. Our findings highlight the critical role of p53 as a tumor suppressor in Burkitt lymphoma and identify MDM4 as a functional target of 1q gain in a wide range of cancers that is therapeutically targetable. SIGNIFICANCE: Targeting MDM4 to alleviate degradation of p53 can be exploited therapeutically across Burkitt lymphoma and other cancers with wild-type p53 harboring 1q gain, the most frequent copy number alteration in cancer.

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