PF-04455242

The drug is a selective KOR antagonist and shows approximately 10- to 20-fold higher affinity for the KOR (K_i = 1–3 nM) over the μ-opioid receptor (MOR) (K_i = 10–64 nM) and has negligible affinity for the δ-opioid receptor (DOR) (K_i > 4,000 nM).^[2][3] It is a "short-acting" or non-inactivating antagonist of the KOR (as opposed to irreversible antagonists like JDTic).^[4] Although originally characterized as a KOR neutral antagonist however, subsequent research revealed in 2020 that PF-04455242 is actually only a moderately efficacious partial antagonist of the KOR (I_max ≈ 50%).^[5] In any case, the drug reversed the analgesic and prolactin-elevating effects of the KOR agonist spiradoline in animals, showed efficacy in animal models predictive of antidepressant activity, and reversed stress-induced reinstatement of cocaine-seeking behavior.^[2][3] However, PF-04455242 also showed a variety of other weak off-target activities.^[2][3]

PF-04455242 reached phase 1 clinical trials for bipolar depression prior to the discontinuation of its development in 2010.^[1][3] Its development was discontinued upon unfavorable toxicological findings in animals that had been exposed to the drug for 3 months.^[2][3] Along with JDTic, which was also discontinued due to toxicity findings early in clinical trials, PF-04455242 was one of the first KOR antagonists to be developed for potential treatment of psychiatric disorders.^[2] It was in phase 1 trials by 2009^[1] and was first described in the scientific literature by 2010.^[6][7][8]

• κ-Opioid receptor § Antagonists
• List of investigational antidepressants