Your search keyword '"Michael Derks"' showing total 13 results

1. Lack of clinically relevant drug-drug interactions when dalcetrapib is co-administered with ezetimibe

Author

Mary Phelan, Michael Derks, and Markus Abt

Subjects

Pharmacology, biology, business.industry, medicine.drug_class, Dalcetrapib, Cmax, Drug interaction, chemistry.chemical_compound, chemistry, Pharmacokinetics, Ezetimibe, Tolerability, Cholesterylester transfer protein, biology.protein, Medicine, Pharmacology (medical), Cholesterol absorption inhibitor, business, medicine.drug

Abstract

WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT • Dalcetrapib, which targets cholesteryl ester transfer protein, is currently in phase III development to evaluate its effect on the prevention of cardiovascular events. It will likely be co-administered with other lipid-modifying drugs such as the cholesterol absorption inhibitor ezetimibe. There are currently no studies on the co-administration of dalcetrapib with ezetimibe. WHAT THIS STUDY ADDS • This study showed no clinically relevant pharmacokinetic interactions when dalcetrapib was co-administered with ezetimibe. The effect of dalcetrapib on raising high-density lipoprotein cholesterol was not compromised, and there was an additive effect on low-density lipoprotein cholesterol lowering with co-administration of dalcetrapib with ezetimibe compared with ezetimibe alone. Dalcetrapib alone or co-administered with ezetimibe was not associated with an increased rate of adverse events compared with ezetimibe alone. AIMS Dalcetrapib, which targets cholesteryl ester transfer protein activity, is in development for prevention of cardiovascular events. Because dalcetrapib will likely be prescribed with other lipid-modifying therapies such as ezetimibe, a study was performed to investigate potential pharmacokinetic interactions between dalcetrapib and ezetimibe. Lipids changes and tolerability were secondary endpoints. METHODS Co-administration of dalcetrapib 900 mg (higher than the phase III dose) with ezetimibe was investigated in a three period, three treatment crossover study in healthy males: 7 days of dalcetrapib, 7 days of dalcetrapib plus ezetimibe, 7 days of ezetimibe alone. A full pharmacokinetic profile was performed on day 7 of each treatment. RESULTS Co-administration of dalcetrapib with ezetimibe was associated with minimal changes in dalcetrapib exposure compared with dalcetrapib alone. Least squares mean ratio (LSMR) (90% confidence interval) was 93.6 (87.1, 100.7) for AUC(0,24 h) and 99.0 (85.2, 115.0) for Cmax. Ezetimibe exposure was reduced with co-administration of ezetimibe with dalcetrapib compared with ezetimibe alone: LSMR 80.3 (74.6, 86.4) for AUC(0,24 h) and 88.9 (80.9, 99.9) for Cmax for total ezetimibe. High-density lipoprotein cholesterol increases associated with co-administration of dalcetrapib with ezetimibe (+29.8%) were comparable with those with dalcetrapib alone (+25.6%), while the reduction in low-density lipoprotein cholesterol with co-administration (−35.9%) was greater than with ezetimibe alone (−20.9%). Dalcetrapib was generally well tolerated when administered alone and when co-administered with ezetimibe. CONCLUSION Co-administration of dalcetrapib with ezetimibe was not associated with clinically significant changes in pharmacokinetic parameters or tolerability and did not diminish the lipid effects of either drug.

Published

2010

2. Coadministration of Dalcetrapib With Pravastatin, Rosuvastatin, or Simvastatin: No Clinically Relevant Drug-Drug Interactions

Author

Graeme Parr, Michael Derks, Mary Phelan, Anne-Marie White, Lynn Turnbull, Nuria Bech, Markus Abt, and Georgina Meneses-Lorente

Subjects

Adult, Male, Simvastatin, Statin, medicine.drug_class, Dalcetrapib, Pharmacology, chemistry.chemical_compound, Cholesterylester transfer protein, Humans, Medicine, Drug Interactions, Pharmacology (medical), Rosuvastatin, Sulfhydryl Compounds, cardiovascular diseases, Rosuvastatin Calcium, Pravastatin, Sulfonamides, Cross-Over Studies, biology, business.industry, Cholesterol, Anticholesteremic Agents, Cholesterol, HDL, nutritional and metabolic diseases, Esters, Cholesterol, LDL, Middle Aged, Amides, Cholesterol Ester Transfer Proteins, Fluorobenzenes, Pyrimidines, chemistry, Area Under Curve, biology.protein, Drug Therapy, Combination, lipids (amino acids, peptides, and proteins), Hydroxymethylglutaryl-CoA Reductase Inhibitors, business, medicine.drug

Abstract

Dalcetrapib targets cholesteryl ester transfer protein and increases high-density lipoprotein cholesterol (HDL-C) levels. It is in clinical development for the prevention of cardiovascular events and will likely be used in combination with standard of care, including statins. Three crossover studies in healthy males investigated the pharmacokinetic drug-drug interaction potential of 900 mg dalcetrapib and statins: two 3-period studies (dalcetrapib plus pravastatin or rosuvastatin) and a 2-period study (dalcetrapib plus simvastatin). Effect on lipids and safety were secondary end points. The 900 mg dose investigated is higher than the 600 mg dose currently being investigated in Phase III. Coadministration of dalcetrapib with pravastatin, rosuvastatin, or simvastatin was not associated with significant increases in statin exposure except for a 26% increase in rosuvastatin C(max) (90% CI 1.088 to 1.468) but not AUC(0-24) (90% CI 0.931 to 1.085). Dalcetrapib AUC(0-24) and C(max) were not significantly altered by coadministration with pravastatin, and were significantly lower when dalcetrapib was coadministered with rosuvastatin or simvastatin compared with dalcetrapib alone. The HDL-C increase with dalcetrapib was not compromised by coadministration with statins, and reduction in low-density lipoprotein cholesterol with dalcetrapib coadministered with statins was greater than with statins alone. Dalcetrapib alone and coadministered with statins was generally well tolerated.

Published

2010

3. No clinically relevant drug–drug interactions when dalcetrapib is co-administered with atorvastatin

Author

Anne-Marie Young, Graeme Parr, Georgina Meneses-Lorente, Michael Derks, Markus Abt, and Mary Phelan

Subjects

Adult, Male, Dalcetrapib, Atorvastatin, Cmax, Pharmacology, Young Adult, chemistry.chemical_compound, Pharmacokinetics, Cholesterylester transfer protein, medicine, Humans, Drug Interactions, Pyrroles, heterocyclic compounds, Pharmacology (medical), Sulfhydryl Compounds, Dosing, Cross-Over Studies, biology, business.industry, Anticholesteremic Agents, nutritional and metabolic diseases, Esters, General Medicine, Middle Aged, Amides, Lipids, Crossover study, Tolerability, chemistry, Heptanoic Acids, biology.protein, Drug Therapy, Combination, lipids (amino acids, peptides, and proteins), Hydroxymethylglutaryl-CoA Reductase Inhibitors, business, medicine.drug

Abstract

Dalcetrapib, which targets cholesteryl ester transfer protein, is in clinical development for prevention of cardiovascular events and is likely to be used concomitantly with statins. Two studies investigated co-administration of dalcetrapib with atorvastatin and any effects of the timing of atorvastatin on the pharmacokinetics of dalcetrapib.Two crossover studies were performed in healthy subjects: a two-period study of dalcetrapib 900 mg concurrently with atorvastatin (concurrent dosing study) and a three-period study of dalcetrapib 600 mg (dose chosen for Phase III) with atorvastatin concurrently or serially 4 h after dalcetrapib (interval dosing study).The primary pharmacokinetic end points were AUC(0 - 24) and C(max); lipid effects and tolerability were secondary end points.In the concurrent study (n = 26), co-administration reduced dalcetrapib AUC(0 - 24) and C(max) and caused small changes in AUC(0 - 24) and C(max) of atorvastatin and its active metabolites. In the interval study (n = 52), serial and concurrent co-administration of atorvastatin resulted in similar reductions in dalcetrapib exposure that were comparable to those observed in the concurrent dosing study. Co-administration did not decrease the efficacy of dalcetrapib or atorvastatin and was generally well tolerated.These results indicate no clinically relevant interactions for co-administration of dalcetrapib with atorvastatin.

Published

2010

4. A single-center, open-label, one-sequence study of dalcetrapib coadministered with ketoconazole, and an in vitro study of the S-methyl metabolite of dalcetrapib

Author

Michael Derks, Olaf Kuhlmann, and Stephen Fowler

Subjects

Adult, Male, medicine.medical_specialty, Antifungal Agents, Adolescent, CYP3A, Dalcetrapib, Metabolite, Administration, Oral, In Vitro Techniques, Pharmacology, Methylation, Drug Administration Schedule, Cohort Studies, Young Adult, chemistry.chemical_compound, Pharmacokinetics, Internal medicine, Cholesterylester transfer protein, medicine, Cytochrome P-450 CYP3A, Humans, Drug Interactions, Pharmacology (medical), Sulfhydryl Compounds, Biotransformation, Aged, biology, CYP3A4, Cholesterol, business.industry, Anticholesteremic Agents, Esters, Middle Aged, Amides, Recombinant Proteins, Ketoconazole, Endocrinology, chemistry, Microsomes, Liver, biology.protein, Cytochrome P-450 CYP3A Inhibitors, business, medicine.drug

Abstract

Background: Dalcetrapib (RO4607381/JTT-705) is currently under clinical investigation for the prevention of cardiovascular events. It inhibits the activity of cholesteryl ester transfer protein and has been reported to increase levels of high-density lipoprotein cholesterol. Objective: Because dalcetrapib is likely to be coadministered with agents that inhibit the cytochrome P450 (CYP) 3A4 isozyme, this study aimed to determine the effect of ketoconazole, a strong CYP3A4 inhibitor, on the pharmacokinetics of dalcetrapib. Methods: An open-label, 1-sequence study was conducted in 2 cohorts of healthy, nonsmoking male volunteers aged 18 through 65 years, with a body mass index of 18 to 32 kg/m 2 . The first cohort received dalcetrapib 600 mg on days 1 and 7 and ketoconazole 400 mg on days 2 through 7, and, based on the results of a planned interim analysis, the second cohort received dalcetrapib 900 mg alone on days 1 and 7 and ketoconazole on days 2 through 7. Pharmacokinetic and safety parameters were assessed at specific times throughout the study. To confirm CYP involvement in the metabolism of the inactive metabolite dalcetrapib- S -methyl, in vitro studies were performed using human liver microsomes and recombinantly expressed CYP isoforms. Results: Of the 26 participants, 96% were white, with a mean age of 38.1 years and a mean weight of 78.6 kg. In the in vivo portion of the study, coadministration of ketoconazole with dalcetrapib 600 mg had no significant effect on any pharmacokinetic parameter of dalcetrapib. Coadministration of ketoconazole with dalcetrapib 900 mg was associated with significant decreases in the dalcetrapib C max (-23%; P = 0.002) and AUC 0-∞ (-18%; P = 0.001) and a significant increase in oral clearance (22%; P = 0.001). Significant increases in the C max ( P = 0.001) and AUC 0-∞ ( P S -methyl were observed with coadministration of ketoconazole. The combination was generally well tolerated, with 32 of 35 adverse events (91.4%) being mild in intensity. The most frequent adverse events were headache (6/26 [23.1%] in the ketoconazole group; 4/18 [22.2%] in the group receiving dalcetrapib 900 mg plus ketoconazole) and diarrhea (4/26 [15.4%] in the ketoconazole group; 2/18 [11.1%] in the group receiving dalcetrapib 900 mg plus ketoconazole). The in vitro studies confirmed the involvement of CYP3A in the metabolism of dalcetrapib- S -methyl. Conclusions: In this clinical study in healthy male volunteers, coadministration of dalcetrapib 600 mg with the CYP3A4 inhibitor ketoconazole was not associated with any significant changes in the pharmacokinetic parameters of the parent compound. Coadministration of dalcetrapib 900 mg with ketoconazole was associated with significant decreases in the dalcetrapib C max and AUC, contrary to the increases that would be expected if dalcetrapib were a substrate for CYP3A4. The combination of dalcetrapib and ketoconazole was generally well tolerated.

Published

2009

5. In vitro and in vivo assessment of the effect of dalcetrapib on a panel of CYP substrates

Author

Stephen Fowler, Michael Derks, and Olaf Kuhlmann

Subjects

Adult, Male, CYP2D6, Adolescent, Dalcetrapib, Pharmacology, Cytochrome P-450 CYP2C8, Rosiglitazone, Young Adult, chemistry.chemical_compound, Clinical Trials, Phase II as Topic, Cytochrome P-450 Enzyme System, Cytochrome P-450 CYP1A2, In vivo, Cytochrome P-450 CYP3A, Humans, Medicine, Sulfhydryl Compounds, Enzyme Inhibitors, CYP2C8, CYP2C9, Aged, Cytochrome P-450 CYP2C9, biology, CYP3A4, business.industry, CYP1A2, Cytochrome P450, Esters, General Medicine, Middle Aged, Amides, Cytochrome P-450 CYP2D6, chemistry, Cardiovascular Diseases, Microsomes, Liver, biology.protein, Drug Therapy, Combination, Thiazolidinediones, Aryl Hydrocarbon Hydroxylases, Hydroxymethylglutaryl-CoA Reductase Inhibitors, business

Abstract

The primary objective of this study was to investigate the drug-drug interaction potential of dalcetrapib on drugs metabolized via major cytochrome P450 (CYP) isoforms using both in vitro and clinical approaches. A secondary objective was to investigate the safety and tolerability of dalcetrapib alone or co-administered either with a combination of five probe drugs or with rosiglitazone.Human liver microsomes and a panel of substrates for CYP enzymes were used to determine IC(50) for inhibition of CYP1A2, CYP2C8, CYP2C9, CYP2C19, CYP2D6, and CYP3A4. In addition, two drug-drug interaction studies were conducted in healthy males: dalcetrapib 900 mg plus the Cooperstown 5 + 1 drug cocktail, which includes substrates for CYP1A2, CYP2C9, CYP2C19, CYP2D6, and CYP3A4, and dalcetrapib 900 mg plus rosiglitazone, a substrate for CYP2C8. Pharmacokinetic and safety parameters were assessed.In vitro, dalcetrapib was inhibitory to all CYP enzymes tested. IC(50) values ranged from 1.5 +/- 0.1 microM for CYP2C8 to 82 +/- 4 microM for CYP2D6. Co-administration of dalcetrapib plus drug cocktail showed no clinically relevant effect of 900 mg dalcetrapib on activity of CYP1A2, CYP2C19, CYP2D6, CYP2C9, or CYP3A4 following repeated administration. Co-administration of dalcetrapib plus rosiglitazone showed no clinically relevant effect of dalcetrapib 900 mg on activity of CYP2C8. Dalcetrapib was generally well tolerated.Although in vitro studies indicated that dalcetrapib inhibits CYP activity, two clinical studies showed no clinically relevant effect on any of the major CYP isoforms at a 900 mg dose, which is higher than the 600 mg dose being explored in phase III studies. Dalcetrapib was generally well tolerated in these studies. However, these studies were limited to a small number of healthy males; additional, larger studies are necessary to study its safety.

Published

2009

6. Effects of food intake on the pharmacokinetic properties of dalcetrapib: findings from three phase I, single-dose crossover studies in healthy volunteers

Author

Georgina Meneses-Lorente, Mary Phelan, Tomohiro Ishikawa, Hitoshi Kawamura, Michael Derks, and Markus Abt

Subjects

Adult, Male, medicine.medical_specialty, Time Factors, Dalcetrapib, Biological Availability, Drug Administration Schedule, chemistry.chemical_compound, Food-Drug Interactions, Young Adult, Pharmacokinetics, Internal medicine, Cholesterylester transfer protein, medicine, Humans, Pharmacology (medical), Sulfhydryl Compounds, Morning, Pharmacology, Meal, Cross-Over Studies, biology, business.industry, Anticholesteremic Agents, digestive, oral, and skin physiology, Esters, Crossover study, Amides, Dietary Fats, Bioavailability, Cholesterol Ester Transfer Proteins, Endocrinology, chemistry, Tolerability, Area Under Curve, biology.protein, business

Abstract

Background Preclinical studies have reported that the relative bioavailability of dalcetrapib, a modulator of cholesteryl ester transfer protein (CETP) inhibitor activity, was ∼60% higher when administered in the fed state compared with the fasting state. Objective This article reports on 3 studies conducted to assess the effects of food intake, timing of administration with respect to meals, and meal size and content on the relative bioavailability of dalcetrapib in healthy male subjects. Methods Three Phase I studies were performed in healthy subjects: (1) a 2-period crossover study of a single dose of dalcetrapib 900 mg administered in the fed and fasting states (fed versus fasting study [1999]); (2) a 3-period crossover study of a single dose of dalcetrapib 600 mg administered after a light morning meal, a standard evening meal, and a light evening meal (meal timing/size study [2005]); and (3) a 4-period crossover study of a single dose of dalcetrapib 600 mg administered 30 minutes after a high-fat meal or a standard evening meal, and 30 minutes before or 3 hours after the latter (high-fat meal study [2007]). Blood samples for pharmacokinetic analyses (AUC 0–36 or AUC 0–∞ , C max ) were collected up to 36, 144, and 96 hours after study drug administration in the fed versus fasting, meal timing/size, and high-fat meal studies, respectively. CETP activity was measured using a radioisotopic method in the fed versus fasting study and a fluorometric method in the meal timing/size and high-fat meal studies. Tolerability was assessed using monitoring of adverse events, laboratory parameters, vital signs, and ECG. Results Six men were enrolled in the fed versus fasting study (mean age, 37 years; mean body mass index [BMI], 23.6 kg/m 2 ). Dalcetrapib exposure was increased by 64% (AUC 0–36 ) and 126% (C max ) after administration in the fed state. Eighteen men were enrolled in the analysis of the effects of meal timing and size on the properties of dalcetrapib (mean age, 30.5 years; mean BMI, 25.1 kg/m 2 ). When dalcetrapib was administered after a light morning or a light evening meal, comparable values were found for mean dalcetrapib AUC 0–∞ (7400 and 7860 ng·h/mL, respectively) and C max (589 and 552 ng/mL), whereas administration after a standard evening meal was associated with increased AUC 0–∞ (14.3%–14.7%) and C max (25.5%–35.3%). Forty-nine men were included in the analysis in the high-fat meal study (mean age, 32.3 years; mean BMI, 23.9 kg/m 2 ). Compared with administration after a standard evening meal, administration after a high-fat evening meal was associated with increased AUC 0–∞ (34.9%) and C max (43.7%). Between-treatment differences in exposure within each study also were reflected in apparent differences in CETP activity. All treatments were generally well tolerated. Conclusions Dalcetrapib exposure was increased in the fed state and, to a lesser extent, was dependent on the size and fat content of the meal. Exposure was independent of dosing time. Dalcetrapib was generally well tolerated.

Published

2011

7. Effect of dalcetrapib, a CETP modulator, on non-cholesterol sterol markers of cholesterol homeostasis in healthy subjects

Author

Andreas Staempfli, David Kallend, Michael Derks, Eric J. Niesor, Denise Blum, and Evelyne Chaput

Subjects

Male, medicine.medical_specialty, Dalcetrapib, Lathosterol, chemistry.chemical_compound, Ezetimibe, Internal medicine, Desmosterol, Cricetinae, Cholesterylester transfer protein, medicine, Animals, Homeostasis, Humans, Sulfhydryl Compounds, Cross-Over Studies, biology, Mesocricetus, Chemistry, Cholesterol, Anticholesteremic Agents, Cholesterol, HDL, Torcetrapib, Phytosterols, Esters, Lipid Metabolism, Amides, Sitosterols, Cholesterol Ester Transfer Proteins, Cholestanol, Endocrinology, Intestinal Absorption, Models, Animal, Intestinal cholesterol absorption, biology.protein, Quinolines, Azetidines, lipids (amino acids, peptides, and proteins), Cardiology and Cardiovascular Medicine, Biomarkers, Switzerland, medicine.drug

Abstract

Subjects with high HDL-C show elevated plasma markers of cholesterol absorption and reduced markers of cholesterol synthesis. We evaluated the effect of dalcetrapib, a cholesteryl ester transfer protein modulator, on markers of cholesterol homeostasis in healthy subjects.Dalcetrapib was administered daily with or without ezetimibe in a randomized, open-label, crossover study in 22 healthy subjects over three 7-day periods: dalcetrapib 900 mg, ezetimibe 10mg, dalcetrapib 900 mg plus ezetimibe 10mg. Plasma non-cholesterol sterols lathosterol and desmosterol (cholesterol synthesis markers) and campesterol, β-sitosterol and cholestanol (intestinal cholesterol absorption markers) were measured. A hamster model was used to compare the effect of dalcetrapib and torcetrapib with or without ezetimibe on these markers and determine the effect of dalcetrapib on cholesterol absorption.Dalcetrapib increased campesterol, β-sitosterol, and cholestanol by 27% (p = 0.001), 32% (p0.001), and 12% (p = 0.03), respectively, in man (non-cholesterol sterol/cholesterol ratio). Dalcetrapib+ezetimibe reduced campesterol by 11% (p = 0.02); β-sitosterol and cholestanol were unaffected. Lathosterol and desmosterol were unchanged with dalcetrapib, but both increased with ezetimibe alone (56-148%, p0.001) and with dalcetrapib + ezetimibe (32-38%, p0.001). In hamsters, dalcetrapib and torcetrapib increased HDL-C by 49% (p = 0.04) and 72% (p = 0.003), respectively. Unlike torcetrapib, dalcetrapib altered cholesterol homeostasis towards increased markers of cholesterol absorption; cholesterol synthesis markers were unaffected by either treatment. Dalcetrapib did not change plasma (3)H-cholesterol level but increased (3)H-cholesterol in plasma HDL vs non-HDL, after oral dosing of labeled cholesterol.Dalcetrapib specifically increased markers of cholesterol absorption, most likely reflecting nascent HDL lipidation by intestinal ABCA1, without affecting markers of synthesis.

Published

2011

8. Safety, tolerability and pharmacokinetics of dalcetrapib following single and multiple ascending doses in healthy subjects: a randomized, double-blind, placebo-controlled, phase I study

Author

Michael Derks, Mary Phelan, Lynn Turnbull, and Judith Anzures-Cabrera

Subjects

Adult, Male, Randomization, Time Factors, Adolescent, Dalcetrapib, Cmax, Pharmacology, Placebo, Models, Biological, Drug Administration Schedule, chemistry.chemical_compound, Electrocardiography, Young Adult, Pharmacokinetics, Double-Blind Method, Medicine, Humans, Pharmacology (medical), Dosing, Sulfhydryl Compounds, Aged, Dose-Response Relationship, Drug, business.industry, Anticholesteremic Agents, Esters, General Medicine, Middle Aged, Amides, Cholesterol Ester Transfer Proteins, Tolerability, chemistry, Pharmacodynamics, Anesthesia, Area Under Curve, business

Abstract

Background: Dalcetrapib is a modulator of cholesteryl ester transfer protein (CETP) activity developed to raise levels of high-density lipoprotein cholesterol (HDL-C) with the goal of further reduction of cardiovascular events additive to standard of care alone. In clinical studies, dalcetrapib has been shown to effectively increase levels of HDL-C with no significant safety concerns. Objective: The primary objective was to investigate the safety of single ascending and multiple ascending doses of dalcetrapib at doses markedly greater than that intended therapeutically (600 mg/day). Secondary objectives were to investigate the pharmacokinetics/pharmacodynamics and dose proportionality of dalcetrapib. Study Design: Randomized, double-blind, placebo-controlled, combined single and multiple ascending dose phase I study. Healthy males (age 18–65 years, body mass index 18–?2) were randomized to four of five dalcetrapib doses (2100,2700, 3300, 3900 or 4500 mg) or placebo, with ≥10 days washout between doses (n= 15, single ascending doses) or to dalcetrapib (1800, 2100, 3000 or 3900 mg once daily) or placebo for 7 days (four cohorts, each n= 10, randomization 8:2, multiple ascending doses). Main Outcome Measure: Tolerability and safety were assessed by monitoring adverse events (AEs), laboratory parameters, vital signs and 12-lead ECG recordings. Primary pharmacokinetic assessments were area under the plasma concentration-time curve (AUC) from time zero to infinity (AUC∞) and maximum observed plasma concentration (Cmax) [single doses] and AUC from time zero to 24 hours (AUC24) and Cmax (multiple doses). Pharmacodynamic assessments included CETP activity and lipids (multiple dosing only). Results: Exposure increased with dose but was less than proportional to increasing dose after single dosing, although deviation from dose proportionality could not be demonstrated for Cmax. Dose proportionality was consistent following multiple doses. Steady state was modelled to have been reached by approximately 4 days, with little to no accumulation. CETP activity reduction was dose dependent (maximum −55% after 3900 mg; placebo −2.6%) at 6 hours post-dose on day 1, while HDL-C increased by 12–19% (placebo −13%) on day 8 following treatment with 1800−3900 mg/day for 7 days. All AEs were mild or moderate in intensity and there were no serious AEs, deaths or withdrawals due to AEs. No clinically relevant effects on laboratory parameters, cardiac parameters or vital signs were noted. Conclusion: Single-dose dalcetrapib up to 4500 mg and multiple doses up to 3900 mg were generally safe and well tolerated.

Published

2011

9. Lack of effect of dalcetrapib on QT interval in healthy subjects following multiple dosing

Author

Georgina Meneses-Lorente, Anne Mwangi, Markus Abt, and Michael Derks

Subjects

Adult, Male, medicine.medical_specialty, Metabolic Clearance Rate, Dalcetrapib, Moxifloxacin, Administration, Oral, Pharmacology, Placebo, QT interval, Drug Administration Schedule, chemistry.chemical_compound, Young Adult, Double-Blind Method, Internal medicine, Cholesterylester transfer protein, Clinical endpoint, Confidence Intervals, Medicine, Humans, Pharmacology (medical), Sulfhydryl Compounds, Aza Compounds, Cross-Over Studies, biology, Dose-Response Relationship, Drug, business.industry, Anticholesteremic Agents, Cholesterol, HDL, Arrhythmias, Cardiac, Esters, Heart, General Medicine, Middle Aged, Amides, Confidence interval, Cholesterol Ester Transfer Proteins, chemistry, Area Under Curve, biology.protein, Cardiology, Electrocardiography, Ambulatory, Quinolines, business, Body mass index, medicine.drug, Fluoroquinolones

Abstract

Evaluate dalcetrapib's potential to prolong QT intervals in healthy subjects.This was a single-center, randomized, active and placebo-controlled, six-sequence, three-period cross-over study. Participants [18-65 years; body mass index (BMI) 18-30 kg/m(2)] were randomized to daily doses of dalcetrapib 600 mg (therapeutic) or 3,900 mg (supratherapeutic) or to dalcetrapib-matched placebo for 7 days. On Day 8, subjects received single-dose moxifloxacin 400 mg (active control) or placebo, following the placebo or dalcetrapib, respectively. Electrocardiographic parameters were recorded on Days -1, 1, 7, and 8. The primary endpoint was the difference to placebo of time-matched change from baseline in the study-specific corrected QT interval (QTcS) at seven time-points within 24 h after dalcetrapib 3,900 mg on Day 7. An upper 95% confidence interval (CI)10 ms confirmed the absence of a significant effect. Pharmacokinetic and lipid-related parameters were measured.Subjects (n = 49) were predominantly male (71%), and all were white, with a mean age of 45 years and mean BMI of 25 kg/m(2). For the primary analysis, the upper 95% CI for dalcetrapib 3,900 mg was10 ms at all time-points. Similar findings were obtained for dalcetrapib 600 mg. Following the administration of moxifloxacin, the QTcS increased by5 ms. At Day 7, exposure for dalcetrapib 3,900 mg was approximately eightfold higher than that for dalcetrapib 600 mg [mean area under the plasma concentration-time curve between time 0 and 24 h 68,500 vs. 8,280 ng*h/mL; mean peak concentration 6,810 vs. 861 ng/mL]. Cholesteryl ester transfer protein activity was inhibited by 30%, and high-density lipoprotein cholesterol increased by 26% for dalcetrapib 600 mg. Dalcetrapib was well tolerated.Dalcetrapib is not associated with QT interval prolongation, even at doses markedly greater than intended therapeutically.

Published

2009

10. Effect of dalcetrapib on non-cholesterol markers of cholesterol homeostasis in healthy subjects and a hamster model

Author

David Kallend, Denise Blum, Eric J. Niesor, Evelyne Chaput, Andreas Staempfli, and Michael Derks

Subjects

medicine.medical_specialty, Cholesterol, business.industry, Dalcetrapib, Healthy subjects, Hamster, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, medicine, Cardiology and Cardiovascular Medicine, business, Cholesterol homeostasis

Published

2011

11. No Clinically Relevant Drug-Drug Interactions Between Dalcetrapib and a Monophasic Oral Contraceptive (Microgynon-30®)

Author

Judith Anzures-Cabrera, Adam Foley-Comer, Michael Derks, and Anne-Marie Young

Subjects

Drug, Nutrition and Dietetics, business.industry, Endocrinology, Diabetes and Metabolism, media_common.quotation_subject, Dalcetrapib, Pharmacology, chemistry.chemical_compound, chemistry, Internal Medicine, Medicine, Cardiology and Cardiovascular Medicine, business, media_common

Published

2010

12. Lack of Clinically Significant Drug−Drug Interactions for Dalcetrapib Coadministered with Atorvastatin

Author

Mary Phelan, Michael Derks, and Markus Abt

Subjects

Drug, Nutrition and Dietetics, business.industry, Endocrinology, Diabetes and Metabolism, media_common.quotation_subject, Dalcetrapib, Atorvastatin, Pharmacology, chemistry.chemical_compound, chemistry, Internal Medicine, Medicine, Cardiology and Cardiovascular Medicine, business, media_common, medicine.drug

Published

2009

13. Dalcetrapib is not Associated with Changes in the QT Interval Following Multiple Doses in Healthy Subjects

Author

Georgina Meneses-Lorente, Michael Derks, Anne Mwangi, and Markus Abt

Subjects

medicine.medical_specialty, Nutrition and Dietetics, business.industry, Endocrinology, Diabetes and Metabolism, Dalcetrapib, Healthy subjects, Multiple dosing, QT interval, chemistry.chemical_compound, chemistry, Internal medicine, Internal Medicine, medicine, Cardiology, Cardiology and Cardiovascular Medicine, business

Published

2009