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Pre-activation of the p53 pathway through Nutlin-3a sensitises sarcomas to drozitumab therapy

journal contribution
posted on 2018-08-03, 00:00 authored by KI Pishas, SJ Neuhaus, MT Clayer, A Adwal, MP Brown, A Evdokiou, DF Callen, Paul NeilsenPaul Neilsen
The present study evaluated the efficacy of drozitumab, a human monoclonal agonistic antibody directed against death receptor 5 (DR5), as a new therapeutic avenue for the targeted treatment of bone and soft-tissue sarcomas. The antitumour activity of drozitumab as a monotherapy or in combination with Nutlin-3a was evaluated in a panel of sarcoma cell lines in vitro and human sarcoma patient samples ex vivo. Knockdown experiments were used to investigate the central role of p53 as a regulator of drozitumab cytotoxicity. Pre-activation of the p53 pathway through Nutlin-3a upregulated DR5, subsequently sensitising sarcoma cell lines and human sarcoma specimens to the pro-apoptotic effects of drozitumab. Silencing of p53 strongly decreased DR5 mRNA expression resulting in abrogation of drozitumab-induced apoptosis. Our study provides the first pre-clinical evaluation of combination therapy using p53-activating agents with drozitumab to further sensitise sarcomas to the cytotoxic effects of DR5 antibody therapy.

Funding

Category 3 - Industry and Other Research Income

History

Volume

30

Issue

1

Start Page

471

End Page

477

Number of Pages

7

eISSN

1791-2431

ISSN

1021-335X

Publisher

Spandidos Publications

Peer Reviewed

  • Yes

Open Access

  • No

External Author Affiliations

University of Adelaide; Royal Adelaide Hospital; Basil Hetzel Institute

Era Eligible

  • Yes

Journal

Oncology Reports

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