Obicetrapib Exhibits Favorable Physiochemical and Pharmacokinetic Properties Compared to Previous Cholesteryl Ester Transfer Protein Inhibitors: An Integrated Summary of Results from Non-human Primate Studies and Clinical Trials

Overview

Journal Pharmacol Res Perspect

Date 2024 Oct 19

PMID 39425271

Authors

Stephen J Nicholls

Adam J Nelson

John J P Kastelein

Marc Ditmarsch

Andrew Hsieh

Judith Johnson

Danielle Curcio

Douglas Kling

Carol F Kirkpatrick

Michael H Davidson

Affiliations

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Abstract

Anacetrapib, a cholesteryl ester transfer protein (CETP) inhibitor previously under development, exhibited an usually extended terminal half-life and large food effect and accumulated in adipose tissue. Other CETP inhibitors have not shown such effects. Obicetrapib, a potent selective CETP inhibitor, is undergoing Phase III clinical development. Dedicated assessments were conducted in pre-clinical and Phase I and II clinical studies of obicetrapib to examine the pharmacokinetic issues observed with anacetrapib. After 9 months of dosing up to 50 mg/kg/day in cynomolgus monkeys, obicetrapib was completely eliminated from systemic circulation and not detected in adipose tissue after a 13-week recovery period. In healthy humans receiving 1-25 mg of obicetrapib, the mean terminal half-life of obicetrapib was 148, 131, and 121 h at 5, 10, and 25 mg, respectively, and food increased plasma levels by ~1.6-fold with a 10 mg dose. At the end of treatment in Phase II trials, mean plasma levels of obicetrapib ranged from 194.5 ng/mL with 2.5 mg to 506.3 ng/mL with 10 mg. Plasma levels of obicetrapib decreased by 92.2% and 98.5% at four and 15 weeks post-treatment, respectively. Obicetrapib shows no clinically relevant accumulation, is minimally affected by food, and has a mean terminal half-life of 131 h for the 10 mg dose. These data support once daily, chronic dosing of obicetrapib in Phase III trials for dyslipidemia management.

Citing Articles

Cholesteryl ester transfer protein inhibition: a pathway to reducing risk of morbidity and promoting longevity.

Davidson M, Hsieh A, Kastelein J Curr Opin Lipidol. 2024; 35(6):303-309.

PMID: 39508067 PMC: 11540282. DOI: 10.1097/MOL.0000000000000955.

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