1. Academic Validation
  2. Single enantiomer of YK-4-279 demonstrates specificity in targeting the oncogene EWS-FLI1

Single enantiomer of YK-4-279 demonstrates specificity in targeting the oncogene EWS-FLI1

  • Oncotarget. 2012 Feb;3(2):172-82. doi: 10.18632/oncotarget.454.
Julie S Barber-Rotenberg 1 Saravana P Selvanathan Yali Kong Hayriye V Erkizan Tara M Snyder S Peter Hong Christina L Kobs Natalie L South Steven Summer Philip J Monroe Maksymilian Chruszcz Veselin Dobrev Perrer N Tosso Lauren J Scher Wladek Minor Milton L Brown Steven J Metallo Aykut Üren Jeffrey A Toretsky
Affiliations

Affiliation

  • 1 Department of Oncology, Georgetown University Lombardi Comprehensive Cancer Center, Washington, DC, USA.
Abstract

Oncogenic fusion proteins, such as EWS-FLI1, are excellent therapeutic targets as they are only located within the tumor. However, there are currently no agents targeted toward transcription factors, which are often considered to be 'undruggable.' A considerable body of evidence is accruing that refutes this claim based upon the intrinsic disorder of transcription factors. Our previous studies show that RNA Helicase A (RHA) enhances the oncogenesis of EWS-FLI1, a putative intrinsically disordered protein. Interruption of this protein-protein complex by small molecule inhibitors validates this interaction as a unique therapeutic target. Single enantiomer activity from a chiral compound has been recognized as strong evidence for specificity in a small molecule-protein interaction. Our compound, YK-4-279, has a chiral center and can be separated into two enantiomers by chiral HPLC. We show that there is a significant difference in activity between the two enantiomers. (S)-YK-4-279 is able to disrupt binding between EWS-FLI1 and RHA in an immunoprecipitation assay and blocks the transcriptional activity of EWS-FLI1, while (R)-YK-4-279 cannot. Enantiospecific effects are also established in cytotoxicity assays and Caspase assays, where up to a log-fold difference is seen between (S)-YK-4-279 and the racemic YK-4-279. Our findings indicate that only one enantiomer of our small molecule is able to specifically target a protein-protein interaction. This work is significant for its identification of a single enantiomer effect upon a protein interaction suggesting that small molecule targeting of intrinsically disordered proteins can be specific. Furthermore, proving YK-4-279 has only one functional enantiomer will be helpful in moving this compound towards clinical trials.

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