Nutlin-3a efficacy in sarcoma predicted by transcriptomic and epigenetic profiling

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hdl_82418.pdf (2.08 MB)
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Date

2014

Authors

Pishas, K.
Neuhaus, S.
Clayer, M.
Schreiber, A.
Lawrence, D.
Perugini, M.
Whitfield, R.
Farshid, G.
Manavis, J.
Chryssidis, S.

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Advisors

Journal Title

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Journal article

Citation

Cancer Research, 2014; 74(3):921-931

Statement of Responsibility

Kathleen I. Pishas, Susan J. Neuhaus, Mark T. Clayer, Andreas W. Schreiber, David M. Lawrence, Michelle Perugini, Robert J. Whitfield, Gelareh Farshid, Jim Manavis, Steve Chryssidis, Bronwen J. Mayo, Rebecca C. Haycox, Kristen Ho, Michael P. Brown, Richard J. D'Andrea, Andreas Evdokiou, David M. Thomas, Jayesh Desai, David F. Callen and Paul M. Neilsen

Conference Name

DOI

10.1158/0008-5472.CAN-13-2424

Abstract

Nutlin-3a is a small-molecule antagonist of p53/MDM2 that is being explored as a treatment for sarcoma. In this study, we examined the molecular mechanisms underlying the sensitivity of sarcomas to Nutlin-3a. In an ex vivo tissue explant system, we found that TP53 pathway alterations (TP53 status, MDM2/MDM4 genomic amplification/mRNA overexpression, MDM2 SNP309, and TP53 SNP72) did not confer apoptotic or cytostatic responses in sarcoma tissue biopsies (n = 24). Unexpectedly, MDM2 status did not predict Nutlin-3a sensitivity. RNA sequencing revealed that the global transcriptomic profiles of these sarcomas provided a more robust prediction of apoptotic responses to Nutlin-3a. Expression profiling revealed a subset of TP53 target genes that were transactivated specifically in sarcomas that were highly sensitive to Nutlin-3a. Of these target genes, the GADD45A promoter region was shown to be hypermethylated in 82% of wild-type TP53 sarcomas that did not respond to Nutlin-3a, thereby providing mechanistic insight into the innate ability of sarcomas to resist apoptotic death following Nutlin-3a treatment. Collectively, our findings argue that the existing benchmark biomarker for MDM2 antagonist efficacy (MDM2 amplification) should not be used to predict outcome but rather global gene expression profiles and epigenetic status of sarcomas dictate their sensitivity to p53/MDM2 antagonists.

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©2013 AACR.

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Grant ID

http://purl.org/au-research/grants/nhmrc/1048132

Published Version

https://doi.org/10.1158/0008-5472.can-13-2424

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Persistent link to this record

http://hdl.handle.net/2440/82418