Thermal profiling reveals phenylalanine hydroxylase as an off-target of panobinostat.
Isabelle BecherThilo WernerCarola DoceEsther A ZaalIna TögelCrystal A KhanAnne RuegerMarcel MuelbaierElsa SalzerCelia R BerkersPaul F FitzpatrickMarcus BantscheffMikhail M SavitskiPublished in: Nature chemical biology (2016)
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.