2015
DOI: 10.1007/s00198-015-3342-4
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Morning vs evening dosing of the cathepsin K inhibitor ONO-5334: effects on bone resorption in postmenopausal women in a randomized, phase 1 trial

Abstract: SummaryThe cathepsin K inhibitor, ONO-5334, improves bone mineral density in postmenopausal women with osteoporosis. The effects of morning versus evening administration of ONO-5334 were investigated by measuring bone turnover marker levels in healthy postmenopausal women. Morning administration of ONO-5334 showed a more consistent suppressive effect on bone resorption than evening administration.IntroductionBone turnover is thought to be subject to circadian variation, and the efficacy of osteoporosis treatme… Show more

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Cited by 7 publications
(5 citation statements)
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“…Two other CatK inhibitors progressed to date to clinical studies: balicatib (Phase 1 and 2 studies) and ONO‐5334 (Phase 1 and 2 studies). PD results from these programmes are generally consistent with the key findings from odanacatib, including: robust reversible inhibition of bone resorption demonstrated by biomarkers and associated with BMD increases; modest reductions of formation biomarkers (small relative to other osteoporosis therapies) at doses with near maximal resorption inhibition, and increased formation biomarkers over baseline at subtherapeutic (very low) dose; transient acceleration of bone resorption on discontinuation of treatment of ≥3 months duration, and osteoclast effects enhancing size, number and/or CatK enzyme levels . Of note, both balicatib and ONO‐5334 were dosed daily in Phase 2, which contrasts with the weekly dosing regimens studied in Phase 2 and 3 for odanacatib.…”
Section: Discussionmentioning
confidence: 99%
“…Two other CatK inhibitors progressed to date to clinical studies: balicatib (Phase 1 and 2 studies) and ONO‐5334 (Phase 1 and 2 studies). PD results from these programmes are generally consistent with the key findings from odanacatib, including: robust reversible inhibition of bone resorption demonstrated by biomarkers and associated with BMD increases; modest reductions of formation biomarkers (small relative to other osteoporosis therapies) at doses with near maximal resorption inhibition, and increased formation biomarkers over baseline at subtherapeutic (very low) dose; transient acceleration of bone resorption on discontinuation of treatment of ≥3 months duration, and osteoclast effects enhancing size, number and/or CatK enzyme levels . Of note, both balicatib and ONO‐5334 were dosed daily in Phase 2, which contrasts with the weekly dosing regimens studied in Phase 2 and 3 for odanacatib.…”
Section: Discussionmentioning
confidence: 99%
“…However, the timing of administration may influence antiresorptive effects due to circadian rhythms in bone turnover, which reach a peak during the night/early morning and a nadir in the late afternoon [ 26 , 27 ]. Eastell et al showed that changes in sCTX inhibition with ONO-5334 SR in morning vs. evening dosing parallel changes in PK [ 30 ]. In addition, the sigmoidal Emax model of sCTX with ONO-5334 SR was similar under fed and fasted conditions [ 29 ].…”
Section: Discussionmentioning
confidence: 99%
“…Therefore, ONO-5334 SR provided a better evaluation of the PK/PD relationship in our previous study [ 29 ]. In an analysis excluding circadian variation of bone resorption markers, the plasma levels of bone resorption markers and ONO-5334 were fitted with sigmoidal maximal inhibitory effect ( Emax ) models, simply reflecting inhibition of cathepsin K. Furthermore, Eastell et al clearly showed that changes in sCTX inhibition with ONO-5334 SR morning vs. evening dosing parallel changes in the PK profile, highlighting a clear link between PK levels and antiresorptive effects [ 30 ].…”
Section: Introductionmentioning
confidence: 99%
“…130 Finally, in a single-blind crossover study examining bone resorption, morning administration of ONO-5334 (a cathepsin K inhibitor) was more effective than evening administration at suppressing C-terminal telopeptide of type I collagen (a marker of bone turnover) across the day. 131 Optimal timing for administration of calcitonin, an antiresorptive hormonal treatment for osteoporosis and Paget's disease, depends on route of administration. For example, 0800 hours or 2100 hours nasal salmon calcitonin treatment transiently reduced bone resorption but did not effectively alter the circadian pattern of bone resorption.…”
Section: Osteoporosismentioning
confidence: 99%
“…A retrospective longitudinal study examining the timing of etidronate administration determined that dosing was similarly effective when taken as single doses across the day if the patient adhered to a 2‐hour fast before and after dosing 130 . Finally, in a single‐blind crossover study examining bone resorption, morning administration of ONO‐5334 (a cathepsin K inhibitor) was more effective than evening administration at suppressing C‐terminal telopeptide of type I collagen (a marker of bone turnover) across the day 131 …”
Section: Endocrine Disordersmentioning
confidence: 99%