QP73

Relevant signaling pathways are identified but off-target effects of the FTO PROTAC degrader QP73 on other m6A modifying proteins and broader profiling outside target family are lacking. A recent paper challenges the current understanding of FB23-2 (a fluorine analog of Dac85) as a selective FTO inhibitor, demonstrating it’s primary action on hDHODH (ACS Pharmacol. Transl. Sci. 2024, 7, 12, 4096–4111). As the selectivity/off-target profile remains underexplored, the compound should be used with caution.

The compound shows a clear time-dependent target degradation. However, selectivity profile has not been performed, so more data is needed despite proof of target engagement. The compound is well-characterised and evidence of ternary complex formation by coimmunoprecipitation assay has been provided. Related compounds and negative control are available. Upper dosing limit is not explored and the concentration at which a hook effect occurs is unknown. The compound has limited usability in vivo as the Cmax is below the DC50 and short half-life is reported (maximum is 1.25 h). Unbound fraction not reported. Nevertheless, immunoblotting demonstrated in vivo target degradation. Without target selectivity and concentration data the compound cannot be recommended as a probe and more validation data is required.