Small molecule selected to disrupt oncogenic protein EWS-FLI1 interaction with RNA Helicase A inhibits Ewing's Sarcoma

Many sarcomas and leukemias carry non-random chromosomal translocations encoding mutant fusion transcription factors that are essential to their molecular pathogenesis. These novel, tumor-specific proteins provides a unique opportunity for the development of highly selective anticancer drugs that ha...

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Autores principales: Erkizan, Hayriye V., Kong, Yali, Merchant, Melinda, Schlottmann, Silke, Barber-Rotenberg, Julie S., Abaan, Ogan D., Chou, Tsu-hang, Dakshanamurthy, Sivanesan, Brown, Milton L., Üren, Aykut, Toretsky, Jeffrey A.
Formato: Texto
Lenguaje:English
Publicado: 2009
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2777681/
https://www.ncbi.nlm.nih.gov/pubmed/19584866
http://dx.doi.org/10.1038/nm.1983
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author Erkizan, Hayriye V.
Kong, Yali
Merchant, Melinda
Schlottmann, Silke
Barber-Rotenberg, Julie S.
Abaan, Ogan D.
Chou, Tsu-hang
Dakshanamurthy, Sivanesan
Brown, Milton L.
Üren, Aykut
Toretsky, Jeffrey A.
author_facet Erkizan, Hayriye V.
Kong, Yali
Merchant, Melinda
Schlottmann, Silke
Barber-Rotenberg, Julie S.
Abaan, Ogan D.
Chou, Tsu-hang
Dakshanamurthy, Sivanesan
Brown, Milton L.
Üren, Aykut
Toretsky, Jeffrey A.
author_sort Erkizan, Hayriye V.
collection PubMed
description Many sarcomas and leukemias carry non-random chromosomal translocations encoding mutant fusion transcription factors that are essential to their molecular pathogenesis. These novel, tumor-specific proteins provides a unique opportunity for the development of highly selective anticancer drugs that has yet to be exploited. A particularly clear example is provided by Ewing's Sarcoma Family Tumors (ESFT) which contain a characteristic t(11;22) translocation leading to expression of the oncogenic fusion protein EWS-FLI1. EWS-FLI1 is a disordered protein that precluded standard structure-based small molecule inhibitor design. Using surface plasmon resonance screening, we discovered a lead compound, NSC635437. A derivative compound, YK-4-279, blocks RHA binding to EWS-FLI1, induces apoptosis in ESFT cells, and reduces the growth of ESFT orthotopic xenografts. These findings provide proof of principle that inhibiting the interaction of mutant cancer-specific transcription factors with the normal cellular binding partners required for their oncogenic activity provides a promising strategy for the development of uniquely effective, tumor-specific anticancer agents.
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spelling pubmed-27776812010-01-05 Small molecule selected to disrupt oncogenic protein EWS-FLI1 interaction with RNA Helicase A inhibits Ewing's Sarcoma Erkizan, Hayriye V. Kong, Yali Merchant, Melinda Schlottmann, Silke Barber-Rotenberg, Julie S. Abaan, Ogan D. Chou, Tsu-hang Dakshanamurthy, Sivanesan Brown, Milton L. Üren, Aykut Toretsky, Jeffrey A. Nat Med Article Many sarcomas and leukemias carry non-random chromosomal translocations encoding mutant fusion transcription factors that are essential to their molecular pathogenesis. These novel, tumor-specific proteins provides a unique opportunity for the development of highly selective anticancer drugs that has yet to be exploited. A particularly clear example is provided by Ewing's Sarcoma Family Tumors (ESFT) which contain a characteristic t(11;22) translocation leading to expression of the oncogenic fusion protein EWS-FLI1. EWS-FLI1 is a disordered protein that precluded standard structure-based small molecule inhibitor design. Using surface plasmon resonance screening, we discovered a lead compound, NSC635437. A derivative compound, YK-4-279, blocks RHA binding to EWS-FLI1, induces apoptosis in ESFT cells, and reduces the growth of ESFT orthotopic xenografts. These findings provide proof of principle that inhibiting the interaction of mutant cancer-specific transcription factors with the normal cellular binding partners required for their oncogenic activity provides a promising strategy for the development of uniquely effective, tumor-specific anticancer agents. 2009-07-05 2009-07 /pmc/articles/PMC2777681/ /pubmed/19584866 http://dx.doi.org/10.1038/nm.1983 Text en http://www.nature.com/authors/editorial_policies/license.html#terms Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Erkizan, Hayriye V.
Kong, Yali
Merchant, Melinda
Schlottmann, Silke
Barber-Rotenberg, Julie S.
Abaan, Ogan D.
Chou, Tsu-hang
Dakshanamurthy, Sivanesan
Brown, Milton L.
Üren, Aykut
Toretsky, Jeffrey A.
Small molecule selected to disrupt oncogenic protein EWS-FLI1 interaction with RNA Helicase A inhibits Ewing's Sarcoma
title Small molecule selected to disrupt oncogenic protein EWS-FLI1 interaction with RNA Helicase A inhibits Ewing's Sarcoma
title_full Small molecule selected to disrupt oncogenic protein EWS-FLI1 interaction with RNA Helicase A inhibits Ewing's Sarcoma
title_fullStr Small molecule selected to disrupt oncogenic protein EWS-FLI1 interaction with RNA Helicase A inhibits Ewing's Sarcoma
title_full_unstemmed Small molecule selected to disrupt oncogenic protein EWS-FLI1 interaction with RNA Helicase A inhibits Ewing's Sarcoma
title_short Small molecule selected to disrupt oncogenic protein EWS-FLI1 interaction with RNA Helicase A inhibits Ewing's Sarcoma
title_sort small molecule selected to disrupt oncogenic protein ews-fli1 interaction with rna helicase a inhibits ewing's sarcoma
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2777681/
https://www.ncbi.nlm.nih.gov/pubmed/19584866
http://dx.doi.org/10.1038/nm.1983
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