Investigating CNS distribution of PF-05212377, a P-glycoprotein substrate, by translation of 5-HT 6 receptor occupancy from non-human primates to humans.
Aarti Sawant-BasakLaigao ChenPeter LockwoodTracey BoydenAngela C DoranJessica MancusoKenneth ZasadnyTimothy McCarthyEvan D MorrisRichard E CarsonIrina EsterlisYiyun HuangNabeel NabulsiBeata PlanetaTerence FullertonPublished in: Biopharmaceutics & drug disposition (2023)
PF-05212377 (SAM760) is a potent and selective 5-HT 6 antagonist, previously under development for the treatment of Alzheimer's disease. In vitro, PF-05212377 was determined to be a P-gp/non-BCRP human transporter substrate. Species differences were observed in the in vivo brain penetration of PF-05212377 with a ratio of the unbound concentration in brain/unbound concentration in plasma (C bu /C pu ) of 0.05 in rat and 0.64 in non-human primates (NHP). Based on pre-clinical evidence, brain penetration and target engagement of PF-05212377 was confirmed in NHP using Positron Emission Tomography (PET) measured 5-HT 6 receptor occupancy (%RO). NHP C pu EC 50 of PF-05212377 was 0.31 nM (consistent with the in vitro human 5HT6 K i : 0.32 nM). P-gp has been reported to be expressed in higher abundance at rat BBB and in similar abundance at BBB of NHP and human; brain penetration of PF-05212377 in humans was postulated to be similar to that in NHP. In humans, PF-05212377 demonstrated dose and concentration dependent increases in 5-HT 6 RO; maximal 5-HT6 RO of ∼80% was measured in humans at doses of ≥15 mg with an estimated unbound plasma EC 50 of 0.37 nM (which was similar to the in vitro human 5HT6 binding K i 0.32 nM). In conclusion, cumulative evidence from NHP and human PET RO assessments confirmed that NHP is more appropriate than rat for the prediction of human brain penetration of PF-05212377, a P-gp/non-BCRP substrate. Clinical trial number: NCT01258751 This article is protected by copyright. All rights reserved.
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