Thermal profiling reveals phenylalanine hydroxylase as an off-target of panobinostat

Publication date

2016-11-01

Authors

Becher, Isabelle
Werner, Thilo
Doce, Carola
Zaal, Esther AORCID 0000-0001-9890-7345ISNI 0000000492962943
Tögel, Ina
Khan, Crystal A.
Rueger, Anne
Muelbaier, Marcel
Salzer, Elsa
Berkers, Celia RISNI 000000038703060X

Editors

Advisors

Supervisors

Document Type

Article
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License

taverne

Abstract

We describe a two-dimensional thermal proteome profiling strategy that can be combined with an orthogonal chemoproteomics approach to enable comprehensive target profiling of the marketed histone deacetylase inhibitor panobinostat. The N-hydroxycinnamide moiety is identified as critical for potent and tetrahydrobiopterin-competitive inhibition of phenylalanine hydroxylase leading to increases in phenylalanine and decreases in tyrosine levels. These findings provide a rationale for adverse clinical observations and suggest repurposing of the drug for treatment of tyrosinemia.

Keywords

Taverne, Molecular Biology, Cell Biology

Citation

Becher, I, Werner, T, Doce, C, Zaal, E A, Tögel, I, Khan, C A, Rueger, A, Muelbaier, M, Salzer, E, Berkers, C R, Fitzpatrick, P F, Bantscheff, M & Savitski, M M 2016, 'Thermal profiling reveals phenylalanine hydroxylase as an off-target of panobinostat', Nature Chemical Biology, vol. 12, no. 11, pp. 908-910. https://doi.org/10.1038/nchembio.2185