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Predictive value and possible applications of human microdosing -=- Berend Oosterhuis, Scientific Director EDS NL PRA International MGTADM 022 T 03 F workshop AGAH 19 April 2008 Contents • Are PK data from microdosing really predictive? – literature overview – CREAM trial – EUMAPP project • Applications of phase 0 microdosing • Conclusions 2 MGTADM 022 T 03 F Overview microdosing literature* Reference Drug Species Method Outcome Lappin & Garner (2003) Nat Drug Discov 2:233 Xceleron 1Aadrenoceptor antagonist oral Human AMS Linear 5-50-500µg Sandhu et al (2004) Drug Metab Dispos 32:1254 Merck Research Labs USA AZT analogue Dog AMS Linear 0.02-1mg Balani et al (2006) Drug Metab Dispos 34:384 Millennium Pharmaceuticals Fluconazole Tolbutamide MLNX Rat LC-MS Linear 0.001-5mg Linear 0.001-5mg Linear 0.01-1mg, 10 mg Cmax, t1/2 linear, AUC non-linear oral+i.v. oral 3 * provided by G Lappin, Xceleron MGTADM 022 T 03 F Overview microdosing literature* 4 Reference Drug Species Method Outcome Yamane et al (2007) J Chromatogr B 858:118 Fexofenadine Human LC-MS Linear 0.1-60mg Vuong et al (2007) J Pharm Sci Vitalea Science Zidovudine Human AMS Linear 520ng- 60mg O’Brien, Z et al Poster presented at AAPS San Diego, Nov 2007 Neurocrine Diphenhydramine Oral+i.v. NBI-1 oral Human AMS Linear 0.1-50mg www.speedel.com Renin inhibitor SPP635 oral+i.v. Human oral * provided by G Lappin, Xceleron MGTADM 022 T 03 F Linear 0.1-10mg AMS Linear 0.1-50mg Overview microdosing literature Trial by Consortium for Resourcing and Evaluating AMS Microdosing (CREAM trial) • Pharmaceutical Companies – – – – Eli Lilly Hoffmann LaRoche Servier Schering AG • Xceleron (AMS) • Pharma Bio-Research (now: PRA International EDS) • Scientific Advisory Board (Prof. Malcolm Rowland, chairman) 5 MGTADM 022 T 03 F CREAM trial: objective and design • Objective – test the ability to predict from microdoses (100 μg) the pharmacokinetics of 5 known drugs at therapeutic doses within acceptable bounds • General design – cross-over designs in 6 subjects per drug (2-way or 3-way) – 14C dose (200 nCi) administered in all periods – 14C-parent and total radioactivity assayed in plasma by AMS – also ‘cold’ assay of parent after pharmacological doses 6 MGTADM 022 T 03 F CREAM trial: overall results 7 MGTADM 022 T 03 F CREAM trial: overall results Drug Was microdose predictive of therapeutic dose? Warfarin CL/F predicted but volume of distribution not predictive oral; 0.1 vs 5 mg ZK253 Schering oral+i.v.; 0.1 vs 50 mg Low oral BA in human predicted i.v. PK predictive within factor of 2 Diazepam i.v. PK predictive i.v.; 0.1 vs 10 mg Midazolam oral+i.v.; 0.1 vs 7.5 mg BA due to 1st pass predictive PK predictive Erythromycin No test (but lessons with acid-labile drugs) oral(+i.v.) 0.1 vs 250 mg 8 MGTADM 022 T 03 F CREAM trial: Warfarin Dose normalized geometric means (n=6) 10000.00 C-14 microdose C-14 therapeutic ng/mL/dose Therapeutic 5 mg T½ = 43 h Parent microdose Parent therapeutic 1000.00 Microdose 100µg T½ ≈ 270 h 100.00 0 20 40 60 80 100 120 Time (h) Clearance/F L/hr Ther 0.26 ; micro 0.21 Literature ~ 0.2 9 MGTADM 022 T 03 F V/F L Ther 17.9 ; micro 42.2 Literature ~ 10 CREAM trial: Midazolam oral microdose versus oral therapeutic dose concentrations dose normalised 10.00 Oral microdose Microdose (100 µg) Plasma concentration measured with HPLC-AMS Oral therapeutic dose ng/mL/dose 1.00 0.10 Therapeutic dose (7.5mg) Plasma concentration measured with LC-MS 0.01 0 10 MGTADM 022 T 03 F 2 4 6 Tim e (h) 8 10 12 14 CREAM trial: Midazolam oral bioavailability of microdose concentrations dose normalised IV microdose Oral microdose Bioavailability = 23% 11 MGTADM 022 T 03 F CREAM trial: Midazolam oral bioavailability of therapeutic dose concentrations dose normalised IV microdose 100 µg Oral therapeutic 7.5mg Bioavailability = 22% 12 MGTADM 022 T 03 F EU Microdose AMS Partnership Program Published on 20 January 2006 MEDICINE, RESEARCH Major injection of EU funds for a microdose project A new EU-funded project kicked off this month which aims to bridge the gap between the laboratory and the clinic. The EU Microdose AMS Partnership Programme (EUMAPP) aims to boost Europe’s expertise in micodosing and its application of AMS, or accelerator mass spectrometry, to developing new candidate drugs ... . . . 13 MGTADM 022 T 03 F EU Microdose AMS Partnership Program Published on 20 January 2006 MEDICINE, RESEARCH Major injection of EU funds for a microdose project A new EU-funded project kicked off this month which aims to bridge the gap between the laboratory and the clinic. The EU Microdose AMS Partnership Programme (EUMAPP) aims to boost Europe’s expertise in micodosing and its application of AMS, or accelerator mass spectrometry, to developing new candidate drugs ... . . . 14 MGTADM 022 T 03 F EU Microdose AMS Partnership Program 15 MGTADM 022 T 03 F Drug Reason for Selection Fexofenadine PgP and OATP substrate Paracetamol Extensive phase II metabolism Phenobarbital Metabolic stability, Long t½ Propafenone CYP 2D6 substrate; Saturable first-pass metabolism Sumatriptan Cytosolic monamine oxidase metabolism S-19812 Formation of non-selective metabolite Clarithromycin CYP-3A4 and PgP substrate EUMAPP: fexofenadine microdose versus therapeutic dose (oral) Mean data, error bars are standard deviation 10 ng/mL per 1 mg dose Oral microdose (100 g) 1 Oral therapeutic dose (120 mg) 0 0 5 Results are dose normalized to 1mg 16 MGTADM 022 T 03 F 10 15 Time (h) Oral micro Oral 120 mg 20 25 EUMAPP: fexofenadine iv microdose with/without oral therapeutic dose IV 14C-microdose (100 g) 10000 1000 pg/mL IV 14C-microdose (100 g) + 120 mg non-labelled oral dose 100 10 0 5 10 15 Time (h) IV micro 17 MGTADM 022 T 03 F IV micro + oral ther 20 25 EUMAPP: fexofenadine absolute oral bioavailability (microdose) 10000 IV 14C-microdose Mean oral absolute bioavailability 38% 1000 pg/mL Oral 14C-microdose 100 10 0 5 10 15 Time (h) Oral micro 18 MGTADM 022 T 03 F IV micro 20 25 EUMAPP: fexofenadine absolute oral bioavailability (therapeutic dose) 100 ng/mL per 1 mg dose IV 14C-microdose + non-labelled 120 mg oral dose Oral therapeutic dose (120 mg) 10 Mean oral absolute bioavailability 28% 1 0 0 5 10 15 Time (h) IV micro + oral ther 19 MGTADM 022 T 03 F Oral 120 mg dose 20 25 Applications of phase 0 microdosing • 14 “Phase 0” microdose studies completed at PRA in last 4 to 5 years – studies with single compound to obtain human PK in case of uncertain or conflicting animal/in vitro PK data – most studies comparing multiple candidates (up to 5) in parallel – design in most studies: parallel panels –> per compound oral-iv crossover in each panel – one 3-way crossover to compare 3 candidates after iv dose in same panel to select best candidate for oral prodrug development – one CYP3A4 “interaction” study to assess influence of ritonavir on clearance of candidate protease inhibitor (1 mg dose) – one study with topical administration on skin (3.8 μg dose) to check if no systemic exposure 20 MGTADM 022 T 03 F Applications of phase 0 microdosing 140 Example from MD study with one compound with uncertain oral BA 5 μg oral dose 120 Concentration (pg/mL) 100 parent Total 14C 80 60 40 20 0 0 12 24 36 Time (Hour) 21 MGTADM 022 T 03 F 48 60 72 Applications of phase 0 microdosing Example from MD study with 5 compounds in iv-oral crossover panels : 10.000 Drug Concentration Compound A – iv 1.000 0.100 0.010 0.001 0 12 24 36 Time (h) Total C-14 (ng equiv/mL) 22 MGTADM 022 T 03 F parent A (ng/mL) 48 Applications of phase 0 microdosing Example from MD study with 5 compounds in iv-oral crossover panels : 10.000 Drug Concentration Compound A – iv+oral 1.000 0.100 0.010 0.001 0 12 24 36 Time (h) Total C-14 (ng equiv/mL) 23 MGTADM 022 T 03 F Parent A (ng/mL) 48 Applications of phase 0 microdosing Example from MD study with 5 compounds in iv-oral crossover panels : Drug concentration 10.000 Compound C – iv 1.000 0.100 0.010 0.001 0 12 24 36 Time (h) Total C-14 (ng equiv/mL) 24 MGTADM 022 T 03 F Parent C (ng/mL) 48 Applications of phase 0 microdosing Example from MD study with 5 compounds in iv-oral crossover panels : 10.000 Drug concentration Compound C – iv+oral 1.000 0.100 0.010 0.001 0 12 24 36 Time (h) Total C-14 (ng equiv/mL) 25 MGTADM 022 T 03 F Parent C (ng/mL) 48 Applications of phase 0 microdosing In February 2005 we successfully completed the first human microdosing studies of new renin inhibitors SPP630 and SPP635 for the treatment of hypertension and for protecting end-organs such as the heart, kidneys and blood vessels. We made significant progress with the development of our SPP600 series by using rational drug design, state-of-the-art preclinical models, and human microdosing to obtain early ADME information, allowing us to ‘screen-in’ the most promising candidates for clinical development. 26 MGTADM 022 T 03 F Applications of phase 0 microdosing Press Releases [2004-07-21 8:03] “The microdosing approach has provided Tripep with pivotal early human PK data on the performance of its candidate drug much more quickly and accurately than would have been possible using conventional development strategies. Encouragingly for the development of alphaHGA, the microdose study has shown 100% oral bioavailability for the candidate, allowing fast-tracking of the molecule into proof-of-concept studies with an enhanced chance of success and significantly reduced risk.” 27 MGTADM 022 T 03 F Applications of phase 0 microdosing Two posters presented the results of a microdosing study in man to assess the pharmacokinetics and the concentrations of AR-709 in key lung compartments in healthy male volunteers. ......... Very importantly AR-709 achieves high concentrations in bronchial mucosa (BM), epithelial lining fluid (ELF) and alveolar macrophages (AM), the three key compartments of the lungs where pathogens can reside and replicate. 28 MGTADM 022 T 03 F Concluding remarks • For the large majority of compounds tested so far (n>20) there was good agreement between PK for microdose versus pharmacological dose • AMS is unique analytical tool; total radioactivity data give added value • Microdosing can help in decision making in early drug development • Small / emerging pharma companies take the lead in applying Phase 0 microdosing for early candidate screening/selection 29 MGTADM 022 T 03 F
