Lengthening the Guanidine–Aryl Linker of Phenylpyrimidinylguanidines Increases Their Potency as Inhibitors of FOXO3-Induced Gene Transcription

[Image: see text] Increased FOXO3 nuclear localization is involved in neuroblastoma chemoresistance and tumor angiogenesis. Accordingly, FOXO3 inhibition is a promising strategy for boosting antitumor immune responses and suppressing FOXO3-mediated therapy resistance in cancer cells. However, no FOX...

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Autores principales: Kohoutova, Klara, Dočekal, Vojtěch, Ausserlechner, Michael J., Kaiser, Nora, Tekel, Andrej, Mandal, Raju, Horvath, Matej, Obsilova, Veronika, Vesely, Jan, Hagenbuchner, Judith, Obsil, Tomas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2022
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9521028/
https://www.ncbi.nlm.nih.gov/pubmed/36188303
http://dx.doi.org/10.1021/acsomega.2c04613
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author Kohoutova, Klara
Dočekal, Vojtěch
Ausserlechner, Michael J.
Kaiser, Nora
Tekel, Andrej
Mandal, Raju
Horvath, Matej
Obsilova, Veronika
Vesely, Jan
Hagenbuchner, Judith
Obsil, Tomas
author_facet Kohoutova, Klara
Dočekal, Vojtěch
Ausserlechner, Michael J.
Kaiser, Nora
Tekel, Andrej
Mandal, Raju
Horvath, Matej
Obsilova, Veronika
Vesely, Jan
Hagenbuchner, Judith
Obsil, Tomas
author_sort Kohoutova, Klara
collection PubMed
description [Image: see text] Increased FOXO3 nuclear localization is involved in neuroblastoma chemoresistance and tumor angiogenesis. Accordingly, FOXO3 inhibition is a promising strategy for boosting antitumor immune responses and suppressing FOXO3-mediated therapy resistance in cancer cells. However, no FOXO3 inhibitors are currently available for clinical use. Nevertheless, we have recently identified (4-propoxy)phenylpyrimidinylguanidine as a FOXO3 inhibitor in cancer cells in the low micromolar range. Here, we report the synthesis and structure–activity relationship study of a small library of its derivatives, some of which inhibit FOXO3-induced gene transcription in cancer cells in a submicromolar range and are thus 1 order of magnitude more potent than their parent compound. By NMR and molecular docking, we showed that these compounds differ in their interactions with the DNA-binding domain of FOXO3. These results may provide a foundation for further optimizing (4-propoxy)phenylpyrimidinylguanidine and developing therapeutics for inhibiting the activity of forkhead box (FOX) transcription factors and their interactions with other binding partners.
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spelling pubmed-95210282022-09-30 Lengthening the Guanidine–Aryl Linker of Phenylpyrimidinylguanidines Increases Their Potency as Inhibitors of FOXO3-Induced Gene Transcription Kohoutova, Klara Dočekal, Vojtěch Ausserlechner, Michael J. Kaiser, Nora Tekel, Andrej Mandal, Raju Horvath, Matej Obsilova, Veronika Vesely, Jan Hagenbuchner, Judith Obsil, Tomas ACS Omega [Image: see text] Increased FOXO3 nuclear localization is involved in neuroblastoma chemoresistance and tumor angiogenesis. Accordingly, FOXO3 inhibition is a promising strategy for boosting antitumor immune responses and suppressing FOXO3-mediated therapy resistance in cancer cells. However, no FOXO3 inhibitors are currently available for clinical use. Nevertheless, we have recently identified (4-propoxy)phenylpyrimidinylguanidine as a FOXO3 inhibitor in cancer cells in the low micromolar range. Here, we report the synthesis and structure–activity relationship study of a small library of its derivatives, some of which inhibit FOXO3-induced gene transcription in cancer cells in a submicromolar range and are thus 1 order of magnitude more potent than their parent compound. By NMR and molecular docking, we showed that these compounds differ in their interactions with the DNA-binding domain of FOXO3. These results may provide a foundation for further optimizing (4-propoxy)phenylpyrimidinylguanidine and developing therapeutics for inhibiting the activity of forkhead box (FOX) transcription factors and their interactions with other binding partners. American Chemical Society 2022-09-14 /pmc/articles/PMC9521028/ /pubmed/36188303 http://dx.doi.org/10.1021/acsomega.2c04613 Text en © 2022 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by/4.0/Permits the broadest form of re-use including for commercial purposes, provided that author attribution and integrity are maintained (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Kohoutova, Klara
Dočekal, Vojtěch
Ausserlechner, Michael J.
Kaiser, Nora
Tekel, Andrej
Mandal, Raju
Horvath, Matej
Obsilova, Veronika
Vesely, Jan
Hagenbuchner, Judith
Obsil, Tomas
Lengthening the Guanidine–Aryl Linker of Phenylpyrimidinylguanidines Increases Their Potency as Inhibitors of FOXO3-Induced Gene Transcription
title Lengthening the Guanidine–Aryl Linker of Phenylpyrimidinylguanidines Increases Their Potency as Inhibitors of FOXO3-Induced Gene Transcription
title_full Lengthening the Guanidine–Aryl Linker of Phenylpyrimidinylguanidines Increases Their Potency as Inhibitors of FOXO3-Induced Gene Transcription
title_fullStr Lengthening the Guanidine–Aryl Linker of Phenylpyrimidinylguanidines Increases Their Potency as Inhibitors of FOXO3-Induced Gene Transcription
title_full_unstemmed Lengthening the Guanidine–Aryl Linker of Phenylpyrimidinylguanidines Increases Their Potency as Inhibitors of FOXO3-Induced Gene Transcription
title_short Lengthening the Guanidine–Aryl Linker of Phenylpyrimidinylguanidines Increases Their Potency as Inhibitors of FOXO3-Induced Gene Transcription
title_sort lengthening the guanidine–aryl linker of phenylpyrimidinylguanidines increases their potency as inhibitors of foxo3-induced gene transcription
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9521028/
https://www.ncbi.nlm.nih.gov/pubmed/36188303
http://dx.doi.org/10.1021/acsomega.2c04613
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