Abstract
BackgroundONO-5334 is a cathepsin K inhibitor that induced bone mineral density (BMD) gain in a phase II study in postmenopausal osteoporosis patients. Even though the antiresorptive effect could only be monitored in the morning during the study, simulation can allow the antiresorptive effect to be assessed over 24 h, with assessment of the relationship to BMD gain.MethodsInhibition of the serum C-telopeptide of type I collagen (sCTX) level at doses of ONO-5334 of 100 mg once daily (QD), 300 mg QD, and 50 mg twice daily (BID) was simulated using plasma ONO-5334 pharmacokinetic (PK) data for repeated dose administration in a phase I study and corresponding sCTX inhibition from the PK-pharmacodynamic (PK/PD) relationship. sCTX was selected because it has a high signal-to-noise ratio compared to other telopeptides. A negative sigmoidal shape for the PK/PD relationship between plasma ONO-5334 and sCTX levels was obtained in our previous study.ResultsThe simulated sCTX inhibition reached >99% of the maximal inhibitory effect (Emax) at 0.5 h in all treatment groups, and decreased to <80% Emax at 8 and 12 h at 50 mg BID and 100 mg QD, respectively. However, sCTX inhibition at 300 mg QD was maintained at ≥82% Emax over 24 h. The mean sCTX inhibition rates for 24 h at 100 mg QD, 300 mg QD and 50 mg BID were 63, 95 and 80% Emax, respectively. There was a positive linear relationship by treatment group between mean sCTX inhibition over 24 h and observed BMD gain in the phase II study.ConclusionThe dose response for BMD with ONO-5334 at 100 and 300 mg QD and higher BMD gain at 50 mg BID vs. 100 mg QD can be explained by sCTX inhibition over 24 h. The simulation gave the antiresorptive effect of ONO-5334 over 24 h and allowed prediction of BMD gain due to ONO-5334.Trial registrationThe registration number in The European Union Clinical Trials Register is 2007–002417-39. The date of registration was August 31, 2007.
Highlights
ONO-5334 is a cathepsin K inhibitor that induced bone mineral density (BMD) gain in a phase II study in postmenopausal osteoporosis patients
From 1.5 to 2 h after administration, plasma ONO-5334 concentrations reached Higher maximum level (Cmax) in the 100 mg Once daily (QD), 300 mg QD and 50 mg Twice daily (BID) groups and were 14, 56, and 4 times higher than the concentration required for 99% Sigmoidal maximal effect (Emax), respectively
This study shows that simulation of antiresorptive effect via serum CTX (sCTX) inhibition provides a quantitative prediction of the dose- and regimen-dependent effects of ONO-5334
Summary
ONO-5334 is a cathepsin K inhibitor that induced bone mineral density (BMD) gain in a phase II study in postmenopausal osteoporosis patients. ONO-5334 is an α-amino acid derivative with a ketone, which differs from another cathepsin K inhibitor, odanacatib, an aliphatic nitrile [18, 19]. These cathepsin K inhibitors have similar efficacy in clinical and non-clinical studies [15, 16, 20,21,22,23,24], but the pharmacokinetic (PK) profiles were differ, with odanacatib developed as a once weekly treatment [18, 25]
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