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  Rational optimization of a transcription factor activation domain inhibitor.

Basu, S., Martínez-Cristóbal, P., Frigolé-Vivas, M., Pesarrodona, M., Lewis, M., Szulc, E., et al. (2023). Rational optimization of a transcription factor activation domain inhibitor. Nature structural & molecular biology, 30(12), 1958-1969. doi:10.1038/s41594-023-01159-5.

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Basu, Shaon, Autor
Martínez-Cristóbal, Paula, Autor
Frigolé-Vivas, Marta, Autor
Pesarrodona, Mireia, Autor
Lewis, Michael, Autor
Szulc, Elzbieta, Autor
Bañuelos, C Adriana, Autor
Sánchez-Zarzalejo, Carolina, Autor
Bielskutė, Stasė, Autor
Zhu, Jiaqi, Autor
Pombo-García, Karina1, Autor           
Garcia-Cabau, Carla, Autor
Zodi, Levente, Autor
Dockx, Hannes, Autor
Smak, Jordann, Autor
Kaur, Harpreet, Autor
Batlle, Cristina, Autor
Mateos, Borja, Autor
Biesaga, Mateusz, Autor
Escobedo, Albert, Autor
Bardia, Lídia, AutorVerdaguer, Xavier, AutorRuffoni, Alessandro, AutorMawji, Nasrin R, AutorWang, Jun, AutorObst, Jon K, AutorTam, Teresa, AutorBrun-Heath, Isabelle, AutorVentura, Salvador, AutorMeierhofer, David1, Autor           García, Jesús, AutorRobustelli, Paul, AutorStracker, Travis H, AutorSadar, Marianne D, AutorRiera, Antoni, AutorHnisz, Denes, AutorSalvatella, Xavier, Autor mehr..
Affiliations:
1Max Planck Institute for Molecular Cell Biology and Genetics, Max Planck Society, ou_2340692              

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 Zusammenfassung: Transcription factors are among the most attractive therapeutic targets but are considered largely 'undruggable' in part due to the intrinsically disordered nature of their activation domains. Here we show that the aromatic character of the activation domain of the androgen receptor, a therapeutic target for castration-resistant prostate cancer, is key for its activity as transcription factor, allowing it to translocate to the nucleus and partition into transcriptional condensates upon activation by androgens. On the basis of our understanding of the interactions stabilizing such condensates and of the structure that the domain adopts upon condensation, we optimized the structure of a small-molecule inhibitor previously identified by phenotypic screening. The optimized compounds had more affinity for their target, inhibited androgen-receptor-dependent transcriptional programs, and had an antitumorigenic effect in models of castration-resistant prostate cancer in cells and in vivo. These results suggest that it is possible to rationally optimize, and potentially even to design, small molecules that target the activation domains of oncogenic transcription factors.

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 Datum: 2023-12-04
 Publikationsstatus: Erschienen
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 Ort, Verlag, Ausgabe: -
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 Art der Begutachtung: -
 Identifikatoren: DOI: 10.1038/s41594-023-01159-5
Anderer: cbg-8675
PMID: 38049566
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Titel: Nature structural & molecular biology
  Andere : Nat Struct Mol Biol
Genre der Quelle: Zeitschrift
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Ort, Verlag, Ausgabe: -
Seiten: - Band / Heft: 30 (12) Artikelnummer: - Start- / Endseite: 1958 - 1969 Identifikator: -