Literature DB >> 24974828

Ewing sarcoma inhibition by disruption of EWSR1-FLI1 transcriptional activity and reactivation of p53.

Wietske van der Ent1, Aart G Jochemsen, Amina F A S Teunisse, S F Gabriel Krens, Karoly Szuhai, Herman P Spaink, Pancras C W Hogendoorn, B Ewa Snaar-Jagalska.   

Abstract

Translocations involving ETS-transcription factors, most commonly leading to the EWSR1-FLI1 fusion protein, are the hallmark of Ewing sarcoma. Despite knowledge of this driving molecular event, an effective therapeutic strategy is lacking. To test potential treatment regimes, we established a novel Ewing sarcoma zebrafish engraftment model allowing time-effective, dynamic quantification of Ewing sarcoma progression and tumour burden in vivo, applicable for screening of single and combined compounds. In Ewing sarcoma the tumour-suppressor gene TP53 is commonly found to be wild-type, thus providing an attractive target for treatment. Here, we study TP53 wild-type (EW7, CADO-ES1 and TC32) and TP53-deleted (SK-N-MC) Ewing sarcoma cell lines to investigate the potentiating effect of p53 reactivation by Nutlin-3 on treatment with YK-4-279 to block transcriptional activity of EWSR1-FLI1 protein. Blocking EWSR1-FLI1 transcriptional activity reduced Ewing sarcoma tumour cell burden irrespective of TP53 status. We show that simultaneous YK-4-279 treatment with Nutlin-3 to stabilize p53 resulted in an additive inhibition of TP53 wild-type Ewing sarcoma cell burden, whilst not affecting TP53-deleted Ewing sarcoma cells. Improved inhibition of proliferation and migration by combinatorial treatment was confirmed in vivo by zebrafish engraftments. Mechanistically, both compounds together additively induced apoptosis of tumour cells in vivo by engaging distinct pathways. We propose reactivation of the p53 pathway in combination with complementary targeted therapy by EWSR1-FLI1 transcriptional activity disruption as a valuable strategy against p53 wild-type Ewing sarcoma.
Copyright © 2014 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

Entities:  

Keywords:  Ewing sarcoma; anti-cancer drug screen; drug synergism; molecular targeted therapy; p53; tumour growth; zebrafish

Mesh:

Substances:

Year:  2014        PMID: 24974828     DOI: 10.1002/path.4378

Source DB:  PubMed          Journal:  J Pathol        ISSN: 0022-3417            Impact factor:   7.996


  22 in total

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Review 3.  Embryonic Zebrafish: Different Phenotypes after Injection of Human Uveal Melanoma Cells.

Authors:  Wietske van der Ent; Claudia Burrello; Mark J de Lange; Pieter A van der Velden; Aart G Jochemsen; Martine J Jager; B Ewa Snaar-Jagalska
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Review 4.  TP53 in bone and soft tissue sarcomas.

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Journal:  Pharmacol Ther       Date:  2019-07-02       Impact factor: 12.310

Review 5.  The Zebrafish model in dermatology: an update for clinicians.

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Journal:  Discov Oncol       Date:  2022-06-17

6.  Inhibition of the oncogenic fusion protein EWS-FLI1 causes G2-M cell cycle arrest and enhanced vincristine sensitivity in Ewing's sarcoma.

Authors:  Stefan K Zöllner; Saravana P Selvanathan; Garrett T Graham; Ryan M T Commins; Sung Hyeok Hong; Eric Moseley; Sydney Parks; Jessica N Haladyna; Hayriye V Erkizan; Uta Dirksen; Michael D Hogarty; Aykut Üren; Jeffrey A Toretsky
Journal:  Sci Signal       Date:  2017-10-03       Impact factor: 8.192

Review 7.  Zebrafish: a new companion for translational research in oncology.

Authors:  Jorge Barriuso; Raghavendar Nagaraju; Adam Hurlstone
Journal:  Clin Cancer Res       Date:  2015-01-08       Impact factor: 12.531

8.  Detection of EWS/FLI-1 fusion in non-Ewing soft tissue tumors.

Authors:  I O Trancău; R Huică; M Surcel; A Munteanu; C Ursaciuc
Journal:  J Med Life       Date:  2014

Review 9.  Sequencing Overview of Ewing Sarcoma: A Journey across Genomic, Epigenomic and Transcriptomic Landscapes.

Authors:  Laurens G L Sand; Karoly Szuhai; Pancras C W Hogendoorn
Journal:  Int J Mol Sci       Date:  2015-07-16       Impact factor: 5.923

10.  Detection of EWS/FLI-1 fusion in non-Ewing soft tissue tumors.

Authors:  I O Trancău; R Huică; M Surcel; A Munteanu; C Ursaciuc
Journal:  J Med Life       Date:  2015 Jan-Mar
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