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4. UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study

Author

Thompson Cd, Maciolek C, Declercq R, Christopher R. Gibson, Tsou Ja, Roger Smith, Wang Yh, Michele Trucksis, Joel A. Klappenbach, Joshua McElwee, Panorchan P, T Laethem, Peggy H. Wong, Jane Harrelson, Vets E, Marian Iwamoto, Peter M. Shaw, John A. Wagner, Gregory J. Opiteck, Garrett Gc, Willson Kj, and Prueksaritanont T

Subjects
Adult, Male, Genotype, Metabolite, Receptors, Antigen, T-Cell, Administration, Oral, Pharmacology, Biology, Minor Histocompatibility Antigens, chemistry.chemical_compound, Glucuronides, Double-Blind Method, Pharmacokinetics, Humans, Pharmacology (medical), Glucuronosyltransferase, Respiratory system, Polymorphism, Genetic, Antagonist, Articles, Metabolism, In vitro, chemistry, Pharmacogenetics, Area Under Curve, Drug Monitoring, Glucuronide, Carbolines, Half-Life
Abstract

MK-7246, an antagonist of the chemoattractant receptor on T helper type 2 (Th2) cells, is being developed for the treatment of respiratory diseases. In a first-in-human study, we investigated whether genetic polymorphisms contributed to the marked intersubject variability in the pharmacokinetics of MK-7246 and its glucuronide metabolite M3. Results from in vitro enzyme kinetic studies suggested that UGT2B17 is probably the major enzyme responsible for MK-7246 metabolism in both the liver and the intestine. As compared with those with the UGT2B17*1/*1 wild-type genotype, UGT2B17*2/*2 carriers, who possess no UGT2B17 protein, had 25- and 82-fold greater mean dose-normalized values of area under the plasma concentration–time curve (AUC) and peak concentration of MK-7246, respectively, and a 24-fold lower M3-to-MK-7246 AUC ratio. The apparent half-life of MK-7246 was not as variable between these two genotypes. Therefore, the highly variable pharmacokinetics of MK-7246 is attributable primarily to the impact of UGT2B17 genetic polymorphisms and extensive first-pass metabolism of MK-7246.

Published
2012

5. UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study

Author

Wang, Y-H, primary, Trucksis, M, additional, McElwee, J J, additional, Wong, P H, additional, Maciolek, C, additional, Thompson, C D, additional, Prueksaritanont, T, additional, Garrett, G C, additional, Declercq, R, additional, Vets, E, additional, Willson, K J, additional, Smith, R C, additional, Klappenbach, J A, additional, Opiteck, G J, additional, Tsou, J A, additional, Gibson, C, additional, Laethem, T, additional, Panorchan, P, additional, Iwamoto, M, additional, Shaw, P M, additional, Wagner, J A, additional, and Harrelson, J C, additional

Published
2012
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6. Suppression of Niacin-induced Vasodilation with an Antagonist to Prostaglandin D2 Receptor Subtype 1.

Author

Lai, E., De Lepeleire, I., Crumley, T. M., Liu, F., Wenning, L. A., Michiels, N., Vets, E., O'Neill, G., Wagner, J. A., and Gottesdiener, K.

Subjects
MEDICAL sciences, VASODILATION, THERAPEUTICS, NIACIN, PATIENTS
Abstract

Niacin (nicotinic acid) reduces cardiovascular events in patients with dyslipidemia. However, symptoms associated with niacin-induced vasodilation (e.g., flushing) have limited its use. Laropiprant is a selective antagonist of the prostaglandin D2 receptor subtype 1 (DP1), which may mediate niacin-induced vasodilation. The aim of this proof-of-concept study was to evaluate the effects of laropiprant (vs placebo) on niacin-induced cutaneous vasodilation. Coadministration of laropiprant 30, 100, and 300 mg with extended-release (ER) niacin significantly lowered flushing symptom scores (by approximately 50% or more) and also significantly reduced malar skin blood flow measured by laser Doppler perfusion imaging. Laropiprant was effective after multiple doses in reducing symptoms of flushing and attenuating the increased malar skin blood flow induced by ER niacin. In conclusion, the DP1 receptor antagonist laropiprant was effective in suppressing both subjective and objective manifestations of niacin-induced vasodilation.Clinical Pharmacology & Therapeutics (2007) 81, 849–857. doi:10.1038/sj.clpt.6100180; published online 28 March 2007 [ABSTRACT FROM AUTHOR]

Published
2007
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7. On-the-road driving performance the morning after bedtime use of suvorexant 15 and 30 mg in healthy elderly.

Author

Vermeeren A, Vets E, Vuurman EF, Van Oers AC, Jongen S, Laethem T, Heirman I, Bautmans A, Palcza J, Li X, Troyer MD, Wrishko R, McCrea J, and Sun H

Subjects
Aged, Aged, 80 and over, Azepines administration & dosage, Cross-Over Studies, Dose-Response Relationship, Drug, Double-Blind Method, Female, Healthy Volunteers, Humans, Male, Sleep Aids, Pharmaceutical administration & dosage, Sleep Initiation and Maintenance Disorders drug therapy, Time Factors, Triazoles administration & dosage, Automobile Driving, Azabicyclo Compounds pharmacology, Azepines pharmacology, Hypnotics and Sedatives pharmacology, Piperazines pharmacology, Psychomotor Performance drug effects, Sleep Aids, Pharmaceutical pharmacology, Triazoles pharmacology
Abstract

Rationale: Suvorexant is a first-in-class orexin receptor antagonist for treating insomnia. There is a general concern that hypnotics may impair next-morning driving ability., Objective: The objective of this study was to evaluate next-morning driving performance in older adults after single and repeated doses of suvorexant., Methods: Double-blind, randomized, placebo-controlled, 4-period crossover study in 24 healthy volunteers (10 females), aged 65-80 years. Subjects were treated with suvorexant (15 and 30 mg) for eight consecutive nights, zopiclone 7.5 mg nightly on days 1 and 8, and placebo. Driving performance was assessed on days 2 and 9 (9 h after dosing) using a 1-h standardized highway driving test in normal traffic, measuring standard deviation of lateral position (SDLP). Drug-placebo differences in SDLP >2.4 cm were considered to reflect clinically meaningful driving impairment., Results: Driving performance as measured by SDLP was not impaired following suvorexant. Mean drug-placebo differences in SDLP following suvorexant 15 and 30 mg on day 2 and 9 were 0.6 cm or less. Their 90 % CIs were all below the threshold of 2.4 cm for clinical relevance and included zero, indicating effects were not clinically meaningful or statistically significant. Symmetry analysis showed no significant differences between the number of participants who had SDLP differences >2.4 cm and those who had SDLP differences <-2.4 cm following suvorexant., Conclusions: There was no clinically meaningful residual effect of suvorexant 15 and 30 mg on next-morning driving (9 h after bedtime dosing) in healthy older adults, as assessed by mean changes in SDLP and by the number of participants on drug versus placebo that exceeded a predetermined threshold for clinically meaningful impairment.

Published
2016
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8. Pharmacokinetics, Safety, and Tolerability of Fevipiprant (QAW039), a Novel CRTh2 Receptor Antagonist: Results From 2 Randomized, Phase 1, Placebo-Controlled Studies in Healthy Volunteers.

Author

Erpenbeck VJ, Vets E, Gheyle L, Osuntokun W, Larbig M, Neelakantham S, Sandham D, Dubois G, Elbast W, Goldsmith P, and Weiss M

Subjects
Administration, Oral, Adult, Dose-Response Relationship, Drug, Double-Blind Method, Female, Half-Life, Humans, Indoleacetic Acids adverse effects, Indoleacetic Acids pharmacokinetics, Male, Middle Aged, Pyridines adverse effects, Pyridines pharmacokinetics, Food-Drug Interactions, Indoleacetic Acids administration & dosage, Pyridines administration & dosage, Receptors, Immunologic antagonists & inhibitors, Receptors, Prostaglandin antagonists & inhibitors
Abstract

We evaluated the pharmacokinetics (PK), safety, and tolerability of a novel oral CRTh2 antagonist, fevipiprant (QAW039), in healthy subjects. Peak concentrations of fevipiprant in plasma were observed 1-3 hours postdosing. Concentrations declined in a multiexponential manner, followed by an apparent terminal phase (t1/2 , ∼20 hours). Steady state was achieved in 4 days with <2-fold accumulation. Elimination was partly by renal excretion (≤30% of the dose) and glucuronidation. Food had minimal impact on the PK of fevipiprant, and it was well tolerated at single and multiple oral doses up to 500 mg/day. No dose-dependent adverse events were observed, and all the events were mild or moderate in severity. Systemic concentrations were sufficiently high to achieve relevant target occupancy, considering in vitro pharmacology data. In summary, the data support further development as a once-daily oral therapy for allergic diseases., (© 2016, The Authors. Clinical Pharmacology in Drug Development Published by Wiley Periodicals, Inc. on behalf of The American College of Clinical Pharmacology.)

Published
2016
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9. Background morbidity in HIV vaccine trial participants from various geographic regions as assessed by unsolicited adverse events.

Author

Schmidt C, Smith C, Barin B, Bakhtyari A, Bart PA, Bekker LG, Chomba E, Clumeck N, Ho D, Hoosen A, Jaoko W, Kaleebu P, Karita E, Keefer MC, van Lunzen J, McMichael A, Mehendale S, Peters B, Ramanathan VD, Robinson A, Rockstroh J, Vardas E, Vets E, Weber J, Graham BS, Than S, Excler JL, Kochhar S, Ho M, Heald A, and Fast PE

Subjects
AIDS Vaccines adverse effects, Adolescent, Adult, Africa South of the Sahara epidemiology, Double-Blind Method, Europe epidemiology, Human Experimentation, Humans, India epidemiology, Male, Middle Aged, Placebos administration & dosage, United States epidemiology, Young Adult, AIDS Vaccines administration & dosage, Cost of Illness, HIV Infections prevention & control
Abstract

Background: Recently, more clinical trials are being conducted in Africa and Asia, therefore, background morbidity in the respective populations is of interest. Between 2000 and 2007, the International AIDS Vaccine Initiative sponsored 19 Phase 1 or 2A preventive HIV vaccine trials in the US, Europe, Sub-Saharan Africa and India, enrolling 900 healthy HIV-1 uninfected volunteers., Objective: To assess background morbidity as reflected by unsolicited adverse events (AEs), unrelated to study vaccine, reported in clinical trials from four continents., Methods: All but three clinical trials were double-blind, randomized, and placebo-controlled. Study procedures and data collection methods were standardized. The frequency and severity of AEs reported during the first year of the trials were analyzed. To avoid confounding by vaccine-related events, solicited reactogenicity and other AEs occurring within 28 d after any vaccination were excluded., Results: In total, 2134 AEs were reported by 76% of all participants; 73% of all events were mild. The rate of AEs did not differ between placebo and vaccine recipients. Overall, the percentage of participants with any AE was higher in Africa (83%) compared with Europe (71%), US (74%) and India (65%), while the percentage of participants with AEs of moderate or greater severity was similar in all regions except India. In all regions, the most frequently reported AEs were infectious diseases, followed by gastrointestinal disorders., Conclusions: Despite some regional differences, in these healthy participants selected for low risk of HIV infection, background morbidity posed no obstacle to clinical trial conduct and interpretation. Data from controlled clinical trials of preventive interventions can offer valuable insights into the health of the eligible population.

Published
2012
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10. Effects of nitazoxanide on pharmacokinetics and pharmacodynamics of a single dose of warfarin.

Author

Vets E, Rossignol JF, and Jackson AS

Subjects
Adolescent, Adult, Antiparasitic Agents administration & dosage, Antiparasitic Agents adverse effects, Cross-Over Studies, Drug Administration Schedule, Drug Interactions physiology, Humans, Male, Middle Aged, Nitro Compounds, Thiazoles adverse effects, Warfarin administration & dosage, Warfarin adverse effects, Thiazoles administration & dosage, Warfarin pharmacokinetics, Warfarin pharmacology
Abstract

Purpose: The effects of nitazoxanide on warfarin pharmacokinetics and pharmacodynamics are examined., Methods: This was a Phase I, single-center, open-label, randomized, two-way, crossover study. Secondary endpoints included an evaluation of the effect of nitazoxanide on coagulation parameters observed after a single dose of warfarin and an assessment of the overall tolerability of study treatments. Fourteen healthy men were selected for the study. The study consisted of two treatment periods (Treatment A and Treatment B), each lasting 6 days, with a washout period of at least 21 days between both warfarin intakes. All subjects were scheduled to receive both Treatment A and Treatment B, according to the randomization list. Treatment A consisted of a single oral dose of 25 mg warfarin sodium (five 5-mg tablets). Treatment B consisted of a single oral intake of 25 mg warfarin sodium (five 5-mg tablets) and one 500-mg tablet of nitazoxanide (with nitazoxanide 500 mg continued twice daily for up to 6 days)., Results: All 14 subjects received Treatment B, and 13 of the 14 subjects received Treatment A. Pharmacokinetic results were similar in both treatments, and pharmacodynamic parameters were similar in both treatments. Fourteen adverse events occurred in eight subjects after administration of at least one dose of the study drug. Eleven adverse events occurred in six subjects after treatment with warfarin and nitazoxanide, and three adverse events occurred in two subjects after treatment with warfarin alone. At discharge, a high hemoglobin level and a low total bilirubin level were reported in both groups., Conclusion: Coadministration of nitazoxanide twice daily for six days did not affect the pharmacokinetic or pharmacodynamic properties of a single 25-mg dose of warfarin sodium. Administration of a single dose of warfarin or combined administration of a single dose of warfarin and multiple doses of nitazoxanide appeared safe and well tolerated.

Published
2009
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11. Assessment of the CYP3A-mediated drug interaction potential of anacetrapib, a potent cholesteryl ester transfer protein (CETP) inhibitor, in healthy volunteers.

Author

Krishna R, Bergman AJ, Jin B, Garg A, Roadcap B, Chiou R, Dru J, Cote J, Laethem T, Wang RW, Didolkar V, Vets E, Gottesdiener K, and Wagner JA

Subjects
Adolescent, Adult, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme Inhibitors, Drug Interactions, Hepatocytes drug effects, Hepatocytes metabolism, Humans, In Vitro Techniques, Ketoconazole pharmacology, Microsomes, Liver drug effects, Microsomes, Liver metabolism, Midazolam pharmacology, Middle Aged, Oxazolidinones adverse effects, Young Adult, Cholesterol Ester Transfer Proteins antagonists & inhibitors, Cytochrome P-450 Enzyme System physiology, Oxazolidinones pharmacology
Abstract

In this study, midazolam was used as a probe-sensitive CYP3A substrate to investigate the effect of anacetrapib on CYP3A activity, and ketoconazole was used as a probe-inhibitor to investigate the effect of potent CYP3A inhibition on the pharmacokinetics of anacetrapib, a novel cholesteryl ester transfer protein inhibitor in development for the treatment of dyslipidemia. Two partially blinded, randomized, 2-period, fixed-sequence studies were performed. Safety, tolerability, and midazolam and anacetrapib plasma concentrations were assessed. All treatments were generally well tolerated. The geometric mean ratios (90% confidence interval) of midazolam with anacetrapib/midazolam alone for AUC0-infinity and Cmax were 1.04 (0.94, 1.14) and 1.15 (0.97, 1.37), respectively. Exposure to anacetrapib was increased by ketoconazole--specifically, the geometric mean ratios (90% confidence interval) of anacetrapib with ketoconazole/anacetrapib alone for AUC0-infinity and Cmax were 4.58 (3.68, 5.71) and 2.37 (2.02, 2.78), respectively. The study showed that anacetrapib does not inhibit or induce CYP3A activity. Furthermore, anacetrapib appears to be a moderately sensitive substrate of CYP3A.

Published
2009
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12. Seasonal influenza vaccine delivered by intradermal microinjection: A randomised controlled safety and immunogenicity trial in adults.

Author

Leroux-Roels I, Vets E, Freese R, Seiberling M, Weber F, Salamand C, and Leroux-Roels G

Subjects
Adolescent, Adult, Antibodies, Viral immunology, Female, Hemagglutinin Glycoproteins, Influenza Virus immunology, Humans, Influenza A Virus, H1N1 Subtype immunology, Influenza A Virus, H3N2 Subtype immunology, Influenza Vaccines adverse effects, Influenza Vaccines immunology, Influenza, Human immunology, Injections, Intradermal, Male, Microinjections, Middle Aged, Vaccination, Vaccines, Inactivated administration & dosage, Vaccines, Inactivated adverse effects, Vaccines, Inactivated immunology, Young Adult, Influenza Vaccines administration & dosage, Influenza, Human prevention & control
Abstract

Influenza vaccines remain largely underused. A promising alternative to current intramuscular vaccines is a trivalent inactivated influenza vaccine (TIV) delivered using a microinjection system to offer a less invasive and possibly more acceptable vaccination. A phase II, multicentre, randomised open-label study in 978 healthy adults (18-57 years) evaluated the immunogenicity and safety of intradermal TIV. Subjects received a 0.1 ml injection of intradermal TIV, containing 9 microg of haemagglutinin (HA) per strain (n = 588) or a conventional 0.5 ml intramuscular vaccine (15 microg of HA/strain; n = 390). Intradermal TIV induced non-inferior humoral immune responses against all three strains and superior responses against both A strains (H1N1, H3N2) compared with the control. Both vaccines were well tolerated.

Published
2008
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13. A phase 1 study to evaluate the safety and immunogenicity of a recombinant HIV type 1 subtype C adeno-associated virus vaccine.

Author

Mehendale S, van Lunzen J, Clumeck N, Rockstroh J, Vets E, Johnson PR, Anklesaria P, Barin B, Boaz M, Kochhar S, Lehrman J, Schmidt C, Peeters M, Schwarze-Zander C, Kabamba K, Glaunsinger T, Sahay S, Thakar M, Paranjape R, Gilmour J, Excler JL, Fast P, and Heald AE

Subjects
AIDS Vaccines adverse effects, Adolescent, Adult, Antibody Formation, Capsid immunology, DNA, Viral administration & dosage, Dependovirus immunology, Double-Blind Method, Female, HIV Infections prevention & control, Humans, Immunity, Cellular, Immunization, Secondary, Injections, Intramuscular, Interferon-gamma blood, Male, Middle Aged, Neutralization Tests, Vaccines, DNA administration & dosage, Vaccines, DNA adverse effects, Vaccines, DNA immunology, Vaccines, Virosome adverse effects, AIDS Vaccines administration & dosage, HIV-1 immunology, T-Lymphocytes immunology, Vaccines, Virosome administration & dosage, gag Gene Products, Human Immunodeficiency Virus immunology
Abstract

A novel prophylactic AIDS vaccine candidate, consisting of single-stranded DNA for HIV-1 subtype C gag, protease, and part of reverse transcriptase genes, enclosed within a recombinant adeno-associated virus serotype-2 protein capsid (tgAAC09) induced T cell responses and antibodies in nonhuman primates. In this randomized, dose escalation phase I trial, HIV-uninfected healthy volunteers (50 in Europe, 30 in India) received a single intramuscular injection of tgAAC09 at 3 x 10(9) DNase resistant particles (DRP) (n = 16), 3 x 10(10) DRP (n = 23), 3 x 10(11) DRP (n = 25), or placebo (n = 16). Twenty-one participants in Europe received a second (boost) dose of 3 x 10(11) DRP tgAAC09 or placebo at least 24 weeks after the first injection. The vaccine was safe and well-tolerated after initial and boost vaccination. Local and systemic reactogenicity was experienced by 13-25% of participants and was not dose related. No vaccine-related serious adverse events were reported. Modest HIV-specific T cell responses were detected in 7/64 vaccinees (40-385 SFC/10(6) PBMC), with 16% (4/25) responders in the highest dose group. All responses were to Gag epitopes. tgAAC09 appears to be safe, well-tolerated, and modestly immunogenic. Further evaluation of higher doses of tgAAC09 and boost injections is ongoing in Africa.

Published
2008
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