Nutlin-3, the Small-molecule Inhibitor of MDM2, Promotes Senescence and Radiosensitises Laryngeal Carcinoma Cells Harbouring Wild-type P53

Overview

Journal Br J Cancer

Specialty Oncology

Date 2010 Jul 1

PMID 20588277

Citations 30

Authors

A K Arya

A El-Fert

T Devling

R M Eccles

M A Aslam

C P Rubbi

N Vlatkovic

J Fenwick

B H Lloyd

D R Sibson

T M Jones

M T Boyd

Affiliations

Soon will be listed here.

Abstract

Background: Primary radiotherapy (RT) is a mainstay of treatment for laryngeal squamous cell carcinoma (LSCC). Although the cure rates for early (T1) vocal cord tumours are high, RT proves ineffective in up to a third of T3 carcinomas. Moreover, RT is associated with debilitating early- and late-treatment-related toxicity, thus finding means to de-escalate therapy, while retaining/augmenting therapeutic effectiveness, is highly desirable. p53 is a key mediator of radiation responses; we therefore investigated whether Nutlin-3, a small-molecule inhibitor of MDM2 (mouse double minute 2; an essential negative regulator of p53), might radiosensitise LSCC cells.

Methods: We performed clonogenic assays to measure radiosensitivity in a panel of LSCC cell lines (for which we determined p53 mutational status) in the presence and absence of Nutlin-3.

Results: LSCC cells harbouring wild-type p53 were significantly radiosensitised by Nutlin-3 (P<0.0001; log-rank scale), and displayed increased cell cycle arrest and significantly increased senescence (P<0.001) in the absence of increased apoptosis; thus, our data suggest that senescence may mediate this increased radiosensitivity.

Conclusion: This is the first study showing Nutlin-3 as an effective radiosensitiser in LSCC cells that retain wild-type p53. The clinical application of Nutlin-3 might improve local recurrence rates or allow treatment de-escalation in these patients.

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