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3. Pharmacokinetics of Sugammadex Dosed by Actual and Ideal Body Weight in Patients With Morbid Obesity Undergoing Surgery

Author

Rebecca E Wrishko, Lata Maganti, Kate Mostoller, Mariëlle van Zutphen-van Geffen, and W. Joseph Herring

Subjects
Adult, Male, 030213 general clinical medicine, Ideal Body Weight, Models, Biological, 030226 pharmacology & pharmacy, Article, Sugammadex, General Biochemistry, Genetics and Molecular Biology, Body Mass Index, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, medicine, Humans, Drug Dosage Calculations, In patient, Dosing, General Pharmacology, Toxicology and Pharmaceutics, Rocuronium, Volume of distribution, Vecuronium Bromide, Dose-Response Relationship, Drug, business.industry, Research, lcsh:Public aspects of medicine, General Neuroscience, lcsh:RM1-950, lcsh:RA1-1270, Articles, General Medicine, Middle Aged, Obesity, Morbid, Neostigmine, lcsh:Therapeutics. Pharmacology, Anesthesia, Neuromuscular Blockade, Female, business, Body mass index, Neuromuscular Nondepolarizing Agents, medicine.drug
Abstract

This analysis of a published study (NCT03346070) evaluated the pharmacokinetics (PKs) of sugammadex dosed by actual body weight (ABW) or ideal body weight (IBW) for reversal of moderate or deep neuromuscular block (M-NMB or D-NMB) in adults with morbid obesity. Adults with body mass index ≥ 40 kg/m2 , ABW ≥ 100 kg, and American Society of Anesthesiologists (ASA) Class 3 were stratified by NMB agent (rocuronium or vecuronium) and randomized 1:1:1:1:1 to (i) M-NMB, sugammadex 2 mg/kg ABW; (ii) M-NMB, sugammadex 2 mg/kg IBW; (iii) M-NMB, neostigmine 5 mg + glycopyrrolate 1 mg; (iv) D-NMB, sugammadex 4 mg/kg ABW; and (v) D-NMB, sugammadex 4 mg/kg IBW. Plasma samples for sugammadex quantification were collected predose, 2, 5, 15, 60, and 120 minutes, and 4, 6 hours postdose. Natural log PK parameters were analyzed using linear fixed effect model with treatment, mode (ABW and IBW), and mode by treatment interaction as fixed terms. The sugammadex PK profile showed rapid distribution followed by monophasic decline consistent with a two-compartment model examined by dose and mode. Absolute sugammadex exposures were ~ 50% higher in the ABW vs. IBW group; dose-independent parameters (clearance and volume of distribution) and terminal half-life remained constant. Sugammadex PK parameter values increased in dose-dependent, linear manner following dosing by ABW or IBW, such that PK continues to be predictive across the clinical dose range. In conjunction with previously published results showing faster recovery with ABW vs. IBW dosing across NMB agent and depth of NMB, these PK findings continue to support dosing by ABW in patients with morbid obesity irrespective of depth of NMB.

Published
2020
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4. Assessment of Bezlotoxumab Immunogenicity

Author

Randolph P. Matthews, Rebecca E Wrishko, Mary Beth Dorr, Diana Montgomery, Lori M. Tobias, and Ka Lai Yee

Subjects
medicine.drug_class, Bacterial Toxins, Repeated dosing, Pharmaceutical Science, Clostridium difficile toxin A, Pharmacology, Monoclonal antibody, 030226 pharmacology & pharmacy, 03 medical and health sciences, Clinical Trials, Phase II as Topic, 0302 clinical medicine, Bacterial Proteins, Humans, Medicine, Pharmacology (medical), Randomized Controlled Trials as Topic, Clinical Trials, Phase I as Topic, biology, business.industry, Immunogenicity, Phase 1 trials, Antibodies, Monoclonal, C difficile, Antibodies, Neutralizing, Anti-Bacterial Agents, Clinical Trials, Phase III as Topic, Bezlotoxumab, 030220 oncology & carcinogenesis, Clostridium Infections, biology.protein, Antibody, business, Broadly Neutralizing Antibodies
Abstract

Bezlotoxumab is a fully human monoclonal antibody that binds and neutralizes Clostridium difficile toxin B. This analysis investigated the potential of bezlotoxumab to induce immunogenicity in healthy phase 1 trial participants and in phase 2/3 trial participants receiving oral antibacterial therapy for primary or recurrent C difficile infection. Immunogenicity to bezlotoxumab was evaluated following a single intravenous dose (≤20 mg/kg) or 2 consecutive doses (10 mg/kg) given 84 days apart in healthy participants across 3 phase 1 trials (Protocol MK-3415A-004, N = 30; Protocol CA-GCDX-05-01, N = 54; Protocol MK-3415A-006, N = 12) and following a single 10 mg/kg dose in 1 phase 2 trial (Protocol CA-GCDX-06-02, ClinicalTrials.gov identifier: NCT00350298; N = 97) and 2 phase 3 trials (Protocols MK-3415A-001 and MK-3415A-002, ClinicalTrials.gov identifiers: NCT01241552 and NCT01513239; N = 1414). No treatment-emergent antidrug antibodies were observed following single or repeated dosing of bezlotoxumab. No phase 1 participants and only 1 phase 2 participant tested positive before bezlotoxumab exposure (non-treatment-emergent positive). Nine participants tested non-treatment-emergent positive in phase 3 trials, 1 of whom was neutralizing antibody-positive. Overall, the immunogenicity potential of bezlotoxumab is considered to be low.

Published
2020
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5. A time-to-event analysis of the exposure–response relationship for bezlotoxumab concentrations and CDI recurrence

Author

Ka Lai Yee, Stefan Zajic, Huub Jan Kleijn, Rebecca E Wrishko, and Mary Beth Dorr

Subjects
Adult, Male, Aging, medicine.medical_specialty, Time Factors, Placebo, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Systemic antibiotics, Recurrence, Internal medicine, medicine, Humans, Exposure response, Survival analysis, Aged, Pharmacology, Sex Characteristics, Models, Statistical, Dose-Response Relationship, Drug, Clostridioides difficile, business.industry, Antibodies, Monoclonal, Middle Aged, Discontinuation, Hospitalization, Treatment Outcome, Bezlotoxumab, Immunoglobulin G, 030220 oncology & carcinogenesis, Charlson comorbidity index, Concomitant, Clostridium Infections, Female, business, Broadly Neutralizing Antibodies
Abstract

Bezlotoxumab is a monoclonal antibody approved for the prevention of recurrent Clostridium difficile infection (rCDI). In a previous exposure–response (E–R) analysis of bezlotoxumab exposure and rCDI, based on data from two phase 3 trials in participants who received placebo or bezlotoxumab 10 mg/kg, rCDI was treated as a binary endpoint and discontinued subjects were imputed as not having rCDI, resulting in an apparent positive E–R trend between rCDI rates and bezlotoxumab exposure. Therefore, a time-to-event (TTE) analysis was applied to investigate the E–R relationship, accounting for the time to rCDI occurrence and participant discontinuation. A TTE model, applying a time-dependent hazard function and right-censoring of data based on rCDI, discontinuation, or study end was developed. Exposure effects and covariates effects were evaluated as predictors affecting the hazard. The TTE model consisted of a Gompertz function with age, endogenous immunoglobulin G to C. difficile toxin B (IgG-B), history of CDI, hospitalization, sex, Charlson Comorbidity Index, and concomitant use of systemic antibiotics affecting the hazard. Exposure effects were characterized with a maximum effect (Emax) E–R relationship on the baseline parameter, and bezlotoxumab exposures achieved at the 10 mg/kg dose were found to be on the plateau of the E–R curve. Endogenous IgG-B significantly impacted the Emax, indicating that low-titer participants derive a greater benefit from bezlotoxumab treatment compared with high-titer participants. The results support the conclusions of the previous E–R analysis, where exposures achieved at the 10 mg/kg dose are on the plateau of the E–R curve.

Published
2020
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6. The Bioequivalence and Effect of Food on the Pharmacokinetics of a Fixed‐Dose Combination Tablet Containing Rosuvastatin and Ezetimibe in Healthy Japanese Subjects

Author

Katsukuni Fujimoto, Rebecca E Wrishko, Yuki Matsumoto, Martin O. Behm, Chisato Nishida, Kenichi Furihata, and Masayoshi Shirakawa

Subjects
Adult, Male, Statin, medicine.drug_class, Hypercholesterolemia, Fixed-dose combination, Administration, Oral, Bioequivalence, Pharmacology, Article, General Biochemistry, Genetics and Molecular Biology, Food-Drug Interactions, Young Adult, Japan, Pharmacokinetics, Ezetimibe, Oral administration, medicine, Humans, Rosuvastatin, Rosuvastatin Calcium, General Pharmacology, Toxicology and Pharmaceutics, Cross-Over Studies, business.industry, lcsh:Public aspects of medicine, Research, Anticholesteremic Agents, General Neuroscience, lcsh:RM1-950, lcsh:RA1-1270, Articles, Fasting, General Medicine, Middle Aged, Postprandial Period, Crossover study, Healthy Volunteers, Drug Combinations, lcsh:Therapeutics. Pharmacology, Therapeutic Equivalency, Drug Therapy, Combination, Female, business, Tablets, medicine.drug
Abstract

Certain patient populations are unable to achieve the recommended low‐density lipoprotein cholesterol goals with statin monotherapy alone. Such patients may benefit from concomitant therapy with ezetimibe (EZE) 10 mg added on to a statin. To this end, fixed‐dose combination (FDC) tablets containing EZE 10 mg and rosuvastatin (ROS) 2.5 mg (EZE/ROS2.5) and EZE 10 mg and ROS 5 mg (EZE/ROS5) have been developed for treatment of hypercholesterolemia. The purpose of the series of clinical studies reported herein was to evaluate the potential food effect (MK‐0653H, protocol 836 (P836)) and the bioequivalence between FDC and co‐administration of EZE and ROS in healthy Japanese subjects under fasted and fed conditions (MK‐0653H, protocol 835 (P835) and MK‐0653H, protocol 846 (P846), respectively). These studies show there is no clinically relevant food effect on EZE exposure following single oral administration of the FDC EZE/ROS5 in healthy Japanese subjects; however, ROS exposure was decreased in the fed state under conditions used to evaluate the maximum food effect. Following single oral administration of individual ROS tablets under the same conditions, the magnitude of decrease in ROS exposure was comparable to that seen with FDC, suggesting that the effect of food on ROS exposure was similar between the FDC tablet and co‐administration of individual EZE and ROS tablets. The FDC EZE/ROS5 was generally well tolerated in healthy Japanese subjects under fasted and fed conditions.

Published
2019
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7. Safety, Tolerability, and Pharmacokinetics of Suvorexant: A Randomized Rising-Dose Trial in Healthy Men

Author

Wen Liu, Deborah Panebianco, Steven Ramael, Rebecca E Wrishko, Ka Lai Yee, Jacqueline B. McCrea, Tamara D. Cabalu, and Nicole Lewis

Subjects
Adult, Male, 0301 basic medicine, Adolescent, Placebo, law.invention, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Pharmacokinetics, Randomized controlled trial, law, medicine, Humans, Pharmacology (medical), Adverse effect, Fatigue, Dose-Response Relationship, Drug, business.industry, Suvorexant, Headache, Azepines, General Medicine, Middle Aged, Triazoles, Healthy Volunteers, Clinical trial, 030104 developmental biology, Tolerability, Area Under Curve, Sleep Aids, Pharmaceutical, Anesthesia, Orexin Receptor Antagonists, medicine.symptom, business, 030217 neurology & neurosurgery, Somnolence
Abstract

Suvorexant (MK-4305) is an orexin receptor antagonist approved for the treatment of insomnia in the USA and other regions. This randomized, double-blind, placebo-controlled, sequential-panel, Phase 1 trial assessed the safety, tolerability, and pharmacokinetic data following single and multiple dosing of suvorexant in healthy men (aged 18–45 years). Within allocated panels, subjects (n = 8) were randomized to receive nightly doses of suvorexant (10, 20, 40, 80, and 100 mg) administered orally for 14 days, or placebo. Safety assessments included daily adverse event (AE) monitoring; pharmacokinetic data were obtained through periodic sampling. Of 40 subjects randomized, 39 completed the trial. The incidence of any AEs in the 10 and 20 mg groups was 67 and 83%, respectively, while 100% of subjects reported AEs in the dose groups of 40, 80, and 100 mg and the placebo group. The most frequently reported AEs were somnolence (n = 19 subjects), fatigue (n = 17), and headache (n = 15). Following single and multiple dosing, median time to reach maximum observed concentration ranged from 1.5 to 4.0 h and the apparent terminal half-life ranged from 7.7 to 14.5 h. Across the investigated doses, accumulation ratios for the area under the concentration–time curve and the maximum observed concentration were independent of dose and ranged from 1.21 to 1.60 and 1.00 to 1.46, respectively. Suvorexant was generally well tolerated after single and multiple dosing for 14 days. The findings support the once-nightly dosing regimen.

Published
2018
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8. Effect of CYP3A Inhibition and Induction on the Pharmacokinetics of Suvorexant: Two Phase I, Open‑Label, Fixed-Sequence Trials in Healthy Subjects

Author

Maria P. Martinez-Cantarin, Walter K. Kraft, Deborah Panebianco, Rebecca E Wrishko, Ka Lai Yee, Eric Mangin, Wen Liu, Jacqueline B. McCrea, and Manu Chakravarthy

Subjects
business.industry, Suvorexant, Cmax, Context (language use), General Medicine, 030204 cardiovascular system & hematology, Pharmacology, 030226 pharmacology & pharmacy, Orexin receptor, Article, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Tolerability, Medicine, Pharmacology (medical), Ketoconazole, Diltiazem, business, medicine.drug
Abstract

BACKGROUND AND OBJECTIVES: Suvorexant is an orexin receptor antagonist indicated for the treatment of insomnia, characterized by difficulties with sleep onset and/or sleep maintenance. As suvorexant is metabolized primarily by Cytochrome P450 3A (CYP3A), and its pharmacokinetics may be affected by CYP3A modulators, the effects of CYP3A inhibitors (ketoconazole or diltiazem) or an inducer (rifampin [rifampicin]) on the pharmacokinetics, safety, and tolerability of suvorexant were investigated. METHODS: In two Phase I, open-label, fixed-sequence trials (Studies P008 and P038), healthy subjects received a single oral dose of suvorexant followed by co-administration with multiple once-daily doses of strong/moderate CYP3A inhibitors (ketoconazole/diltiazem) or a strong CYP3A inducer (rifampin). Treatments were administered in the morning: suvorexant 4 mg with ketoconazole 400 mg (Study P008; N = 10), suvorexant 20 mg with diltiazem 240 mg (Study P038; N = 20), and suvorexant 40 mg with rifampin 600 mg (Study P038; N = 10). Area under the plasma concentration–time curve from time zero to infinity (AUC(0–∞)), maximum plasma concentration (C(max)), half-life (t(½)), and time to C(max) (t(max)) were derived from plasma concentrations of suvorexant collected at prespecified time points up to 10 days following CYP3A inhibitor/inducer co-administration. Adverse events (AEs) were recorded. RESULTS: Co-administration with ketoconazole resulted in increased exposure to suvorexant [AUC(0–∞): geometric mean ratio (GMR); 90% confidence interval (CI) 2.79 (2.35, 3.31)] while co-administration with diltiazem resulted in a lesser effect [GMR (90% CI): 2.05 (1.82, 2.30)]. Co-administration with rifampin led to a marked decrease (88%) in suvorexant exposure. Consistent with morning administration and known suvorexant pharmacology, somnolence was the most frequently reported AE. CONCLUSIONS: These results are consistent with expectations that strong CYP3A inhibitors and inducers exert marked effects on suvorexant pharmacokinetics. In the context of a limited sample size, single suvorexant doses were generally well tolerated in healthy subjects when co-administered with/without a CYP3A inhibitor/inducer.

Published
2019

9. Effect of Vorapaxar Alone and in Combination with Aspirin on Bleeding Time and Platelet Aggregation in Healthy Adult Subjects

Author

Ulhas P. Naik, Srikanth Nagalla, Matt S. Anderson, Jocelyn Gilmartin, Brittany Walker, Walter K. Kraft, Sandra Zhang, Ferdous Gheyas, Derek L Chappell, Jay Horrow, and Rebecca E Wrishko

Subjects
Adult, Male, Bleeding Time, Platelet Aggregation, Pyridines, 030204 cardiovascular system & hematology, 030226 pharmacology & pharmacy, Article, General Biochemistry, Genetics and Molecular Biology, law.invention, Lactones, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Pharmacotherapy, Randomized controlled trial, law, Bleeding time, Humans, Medicine, General Pharmacology, Toxicology and Pharmaceutics, Vorapaxar, Blood coagulation test, Aspirin, Arachidonic Acid, medicine.diagnostic_test, business.industry, Research, General Neuroscience, Antagonist, Articles, General Medicine, Middle Aged, Healthy Volunteers, Adenosine Diphosphate, Regimen, Anesthesia, Drug Therapy, Combination, Female, Receptors, Thrombin, Blood Coagulation Tests, business, medicine.drug
Abstract

The effect of the protease-activated receptor-1 (PAR-1) antagonist vorapaxar on human bleeding time is not known. This was a randomized, two-period, open-label trial in healthy men (n = 31) and women (n = 5). In period 1, subjects received 81 mg aspirin q.d. or a vorapaxar regimen achieving steady-state plasma concentrations equivalent to chronic 2.5 mg q.d. doses, for 7 days. In period 2, each group added 7 days of the therapy alternate to that of period 1 without washout. Bleeding time and platelet aggregation using arachidonic acid, ADP, and TRAP agonists were assessed. Bleeding time geometric mean ratio (90% CI) for vorapaxar/baseline was 1.01 (0.88-1.15), aspirin/baseline was 1.32 (1.15-1.51), vorapaxar + aspirin/vorapaxar was 1.47 (1.26-1.70), and vorapaxar + aspirin/aspirin was 1.12 (0.96-1.30). Unlike aspirin, vorapaxar did not prolong bleeding time compared with baseline. Bleeding time following administration of vorapaxar with aspirin was similar to that following aspirin alone.

Published
2016
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11. On-the-Road Driving Performance the Morning after Bedtime Use of Suvorexant 20 and 40 mg

Author

T Laethem, Cees J Van Leeuwen, Xiadong Li, Annemiek Vermeeren, An Bautmans, Rebecca E Wrishko, Eric F. P. M. Vuurman, John Palcza, Anita C M Van Oers, Hong Sun, Stefan Jongen, Jacqueline B. McCrea, Matthew D. Troyer, Ingeborg Heirman, Section Psychopharmacology, RS: FPN NPPP II, Onderzoeksondersteuning, and RS: FSE MSP

Subjects
Male, Individuality, Poison control, ALCOHOL, DSST, hypnotics, Piperazines, memory, Medicine, Morning, Netherlands, Zopiclone, Cross-Over Studies, INSOMNIA PATIENTS, PLACEBO, ZOLPIDEM, Azepines, Middle Aged, IMPAIRMENT, Healthy Volunteers, Anesthesia, Female, Sleep Stages, medicine.drug, Sleep Aids, Adult, medicine.medical_specialty, Automobile Driving, plasma concentrations, Placebo, Bedtime, OREXIN RECEPTOR ANTAGONIST, Morning Driving Performance after Bedtime Use of Suvorexant, Young Adult, Double-Blind Method, Physiology (medical), driving, Humans, Dosing, business.industry, Suvorexant, suvorexant, balance, Triazoles, ZOPICLONE 7.5 MG, Crossover study, SLEEP, Surgery, Sleep Aids, Pharmaceutical, orexin antagonist, Pharmaceutical, zopiclone, Neurology (clinical), Self Report, business, Azabicyclo Compounds, Psychomotor Performance
Abstract

Study Objective: To evaluate next-morning driving performance in adults younger than 65 years, after single and repeated doses of suvorexant 20 and 40 mg. Design: Double-blind, placebo-controlled, 4-period crossover study. Setting: Maastricht University, The Netherlands. Participants: 28 healthy volunteers (15 females), aged 23 to 64 years. Interventions: Suvorexant (20 and 40 mg) for 8 consecutive nights; zopiclone 7.5 mg nightly on day 1 and 8; placebo. Measurements: Performance on day 2 and 9 (9 h after dosing) using a one-hour standardized highway driving test in normal traffic, measuring standard deviation of lateral position (SDLP). Drug-placebo changes in SDLP > 2.4 cm were considered to reflect meaningful driving impairment. Results: Mean drug-placebo changes in SDLP following suvorexant 20 and 40 mg were 1.01 and 1.66 cm on day 2, and 0.48 and 1.31 cm on Day 9, respectively. The 90% CIs of these changes were all below 2.4 cm. Symmetry analysis showed that more subjects had SDLP changes > 2.4 cm than < -2.4 cm following suvorexant 20 and 40 mg on day 2, and following suvorexant 40 mg on day 9. Four female subjects requested that a total of 5 driving tests-all following suvorexant-stop prematurely due to self-reported somnolence. Conclusions: As assessed by mean changes in standard deviation of lateral position (SDLP), there was no clinically meaningful residual effect of suvorexant in doses of 20 and 40 mg on next-morning driving (9 h after bedtime dosing) in healthy subjects < 65 years old. There may be some individuals who experience next-day effects, as suggested by individual changes in SDLP and prematurely stopped tests.

Published
2015
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12. Pharmacokinetics of sugammadex in subjects with moderate and severe renal impairment

Author

Christina Reitmann, Dennis Wolford, Kenneth C. Lasseter, David E. Gutstein, Rebecca E Wrishko, William D. Hanley, Joanna Udo de Haes, K Chris Min, and Thomas Marbury

Subjects
Male, Cmax, Renal function, Kidney, urologic and male genital diseases, Saline flush, Sugammadex, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, 030202 anesthesiology, Humans, Medicine, Pharmacology (medical), Renal Insufficiency, Rocuronium, Adverse effect, Aged, Pharmacology, business.industry, Kidney metabolism, 030208 emergency & critical care medicine, Middle Aged, Case-Control Studies, Anesthesia, Neuromuscular Blockade, Female, business, Half-Life, gamma-Cyclodextrins, medicine.drug
Abstract

AIMS Sugammadex rapidly reverses moderate and deep rocuronium- or vecuronium-induced neuromuscular blockade at doses of 4 mg/kg and 2 mg/kg, respectively. Sugammadex is renally eliminated. This study evaluated the pharmacokinetics of sugammadex in subjects with renal impairment versus those with normal renal function. METHODS This open-label, two-part, phase 1 study included adults with moderate (creatinine clearance (CLcr) 30

Published
2017
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13. 1558. A Population Pharmacokinetic Model for Posaconazole Intravenous Solution and Oral Powder for Suspension Formulations in Pediatric Patients With Neutropenia

Author

Rebecca E Wrishko, Rik de Greef, Hetty Waskin, Christopher Bruno, Eric Mangin, and Gregory A. Winchell

Subjects
education.field_of_study, medicine.medical_specialty, Posaconazole, business.industry, Population, Oral Powder, Neutropenia, Powder dose form, medicine.disease, Gastroenterology, Abstracts, Infectious Diseases, Oncology, Pharmacokinetics, Internal medicine, Poster Abstracts, medicine, education, business, medicine.drug, Biological availability, Clearance
Abstract

Background Posaconazole is approved in adults for prophylaxis and treatment of invasive fungal disease. Two formulations that offer weight-based dosing—intravenous (IV) and oral powder for suspension (PFS)—are being evaluated in children. A population pharmacokinetic (popPK) approach was used to characterize and predict the PK exposure of posaconazole PFS and IV formulations in children to identify dosages associated with achieving a target PK of 1200 ng/mL as the mean Cavg and individual Cavg ≥500 ng/mL and Methods A popPK model was developed through nonlinear mixed-effects modeling using data obtained from a trial in children with neutropenia (ClinicalTrials.gov, NCT02452034; Merck protocol, MK-5592-097). Three dose cohorts (3.5, 4.5, and 6 mg/kg/day [≤300 mg/day]) were studied in two age groups (2– Results An open one-compartmental PK model with first-order absorption and estimated bioavailability, as well as allometrically scaled effects of body weight on clearance and volume, adequately described the PK of posaconazole IV and PFS formulations. Model predictions are shown in the Table. Effects of the different food covariates were not statistically significant. Simulations indicated that for the 6-mg/kg/d dose, model-predicted Cavg generally met PK targets. Model-predicted Cavg was ≥500 ng/mL in >90% of subjects in all cohorts. The 1200-ng/mL target geometric mean Cavg was achieved for all but the 2– Conclusion This popPK-based analysis demonstrated that the 6-mg/kg/d dose of IV or PFS posaconazole formulation (≤300 mg/days) is appropriate for children (2–17 years) and that PFS can be administered without regard to food. Disclosures All authors: No reported disclosures.

Published
2019
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14. On-the-road driving performance the morning after bedtime use of suvorexant 15 and 30 mg in healthy elderly

Author

Matthew D. Troyer, Ingeborg Heirman, Anita C M Van Oers, Hong Sun, Annemiek Vermeeren, An Bautmans, Rebecca E Wrishko, John Palcza, Xiadong Li, T Laethem, Jacqueline B. McCrea, Eric F. P. M. Vuurman, Eva Vets, Stefan Jongen, Section Psychopharmacology, RS: FPN NPPP II, Onderzoeksondersteuning, and RS: FSE MSP

Subjects
Male, PSYCHOMOTOR PERFORMANCE, Time Factors, Poison control, ALCOHOL, Piperazines, 0302 clinical medicine, Elderly, Sleep Initiation and Maintenance Disorders, Insomnia, Hypnotics and Sedatives, Medicine, Original Investigation, Morning, Aged, 80 and over, Zopiclone, Cross-Over Studies, PLACEBO, Azepines, Healthy Volunteers, Orexin receptor, Female, TRIAL, medicine.symptom, medicine.drug, Driving, Automobile Driving, medicine.medical_specialty, Orexin antagonist, Bedtime, OREXIN RECEPTOR ANTAGONIST, 03 medical and health sciences, Double-Blind Method, mental disorders, Humans, VOLUNTEERS, Psychiatry, Aged, Pharmacology, Dose-Response Relationship, Drug, business.industry, Suvorexant, MEMORY, Triazoles, ZOPICLONE 7.5 MG, SLEEP, 030227 psychiatry, INSOMNIA, Sleep Aids, Pharmaceutical, business, Azabicyclo Compounds, 030217 neurology & neurosurgery, Hypnotics
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

Published
2016

15. Abstract 527: Vorapaxar Does Not Increase Bleeding Time

Author

Matt S. Anderson, Rebecca E Wrishko, Jocelyn Gilmartin, Srikanth Nagalla, Walter K. Kraft, Derek L Chappell, Sandra Zhang, and Uhlas P Naik

Subjects
Aspirin, medicine.diagnostic_test, business.industry, medicine.disease, Thrombosis, Clinical trial, Regimen, Bleeding time, Anesthesia, medicine, Coagulation testing, Myocardial infarction, Cardiology and Cardiovascular Medicine, business, medicine.drug, Vorapaxar
Abstract

Vorapaxar is a novel PAR-1 inhibitor approved in the US and EU to reduce risk of thrombotic CV events in patients with a history of MI, and in the US also in patients with PAD. It does not affect coagulation tests (TT, PT, aPTT, ACT, ECT). Aspirin and P2Y 12 inhibitors prolong human bleeding time (BT); does vorapaxar? Methods: In this randomized, active controlled, parallel group, 2-period, single-blind, open-label trial, healthy men (n=31) and women (n=5), in Period 1, received either 81 mg aspirin (ASA) QD for 7 days (N=18), or a 7 day regimen of vorapaxar (N=18) achieving steady state plasma concentrations equivalent to chronic 2.5 mg QD doses. In Period 2, each group added 7 days of the therapy alternate to that of Period 1 without washout. BT and platelet aggregation (PA) using arachidonic acid, ADP, and TRAP agonists were collected predose in Periods 1 (baseline) and 2, and 24 h after Period 2 last dose. A linear mixed effects model with fixed effect for treatment analyzed data. Results: BT geometric mean ratio (90% CI) for (vorapaxar/baseline) was 1.01 (0.88, 1.15), (ASA/baseline) was 1.32 (1.15, 1.51), (vorapaxar+ASA/vorapaxar) was 1.47 (1.26, 1.70), (vorapaxar+ASA/ASA) was 1.12 (0.96, 1.30). Each antiplatelet inhibited PA only as expected. See figure. Conclusions: Unlike ASA, vorapaxar did not prolong BT compared to baseline. When given with ASA, there is a slight numerical increase in BT beyond that of ASA. Implications for clinical spontaneous or surgical bleeding await further analyses of clinical trial data.

Published
2016
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16. Relationship Between Exposure to Prasugrel Active Metabolite and Clinical Outcomes in the TRITON-TIMI 38 Substudy

Author

Rebecca E. Wrishko, William L. Macias, C. Steven Ernest, Jeffrey S. Riesmeyer, Shashank Rohatagi, Daniel E. Salazar, David S. Small, Govinda Weerakkody, Junxiang Luo, Ying G. Li, and Lan Ni

Subjects
Male, medicine.medical_specialty, Prasugrel, Population, Hemorrhage, Thiophenes, Logistic regression, Models, Biological, Severity of Illness Index, Piperazines, Double-Blind Method, Pharmacokinetics, Internal medicine, Post-hoc analysis, medicine, Humans, Prodrugs, Pharmacology (medical), Acute Coronary Syndrome, education, Biotransformation, Active metabolite, Aged, Pharmacology, education.field_of_study, Dose-Response Relationship, Drug, business.industry, Incidence, Incidence (epidemiology), Body Weight, Age Factors, Thrombosis, Receptors, Purinergic P2Y12, Surgery, surgical procedures, operative, Purinergic P2Y Receptor Antagonists, business, Prasugrel Hydrochloride, Platelet Aggregation Inhibitors, TIMI, medicine.drug
Abstract

In TRITON-TIMI 38, levels of the prasugrel active metabolite (pras-AM) were measured in a population pharmacokinetic substudy that characterized the intrinsic and extrinsic factors influencing exposure. Higher exposure to the pras-AM was observed in low-weight or very elderly patients. The authors hypothesized that this higher exposure might explain the higher risk of non–coronary artery bypass graft (CABG)– related TIMI-related bleeding observed in these 2 patient populations. The relationship between estimated exposure to the pras-AM and clinical outcomes was assessed in 1159 prasugrel-treated patients enrolled in the substudy using multivariable logistic regression analysis. There was no relationship between pras-AM exposure and efficacy through 3 days or after 3 days. Higher estimated pras-AM exposure was associated with a higher incidence of non-CABG-related TIMI major or minor bleeding after 3 days (P � .05) but not through 3 days from start of study drug. Factors associated with increased risk for non-CABG-related TIMI bleeding (t75 years and � 60 kg) also identified subgroups with higher exposure to the pras-AM. Within low body weight and very elderly subgroups, bleeding was largely confined to patients having the highest exposure to the pras-AM, indicating that a prasugrel lower dose in these subgroups may reduce the risk of bleeding while maintaining efficacy.

Published
2012
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17. Population Pharmacokinetic Analyses to Evaluate the Influence of Intrinsic and Extrinsic Factors on Exposure of Prasugrel Active Metabolite in TRITON-TIMI 38

Author

Ying G. Li, Lan Ni, Shashank Rohatagi, Jeffrey R. Riesmeyer, Eugene Braunwald, Elliott M. Antman, Rebecca E. Wrishko, C. Steven Ernest, William L. Macias, David S. Small, Daniel E. Salazar, Govinda Weerakkody, and Stephen D. Wiviott

Subjects
Adult, Male, medicine.medical_specialty, Prasugrel, Population, Renal function, Thiophenes, Pharmacology, Models, Biological, Gastroenterology, Piperazines, Pharmacokinetics, Internal medicine, Diabetes mellitus, medicine, Humans, Prodrugs, Pharmacology (medical), education, Active metabolite, Aged, Randomized Controlled Trials as Topic, Aged, 80 and over, education.field_of_study, Chemistry, Body Weight, Age Factors, Middle Aged, medicine.disease, Confidence interval, Clinical Trials, Phase III as Topic, Linear Models, Female, Prasugrel Hydrochloride, Body mass index, Platelet Aggregation Inhibitors, medicine.drug
Abstract

Serial pharmacokinetic (PK) sampling in 1159 patients from TRITON-TIMI 38 was undertaken. A multilinear regression model was used to quantitatively predict prasugrel's active metabolite (Pras-AM) concentrations from its 2 downstream inactive metabolites. Population-based methods were then applied to Pras-AM concentration data to characterize the PK. The potential influence of body weight, body mass index, age, sex, renal function, diabetes, tobacco use, and other disease status on Bayesian estimates of Pras-AM exposures was assessed. The PK of Pras-AM was adequately described by a multicompartmental model and consistent with results from previous studies. The systemic exposure of prasugrel was not appreciably affected by body mass index, gender, diabetes, smoking, and renal impairment. Pras-AM mean exposure in patients weighing60 kg (4.1%) was 30% (90% confidence interval [CI] 1.16-1.45) higher than exposure in patientsor =60 kg. Mean Pras-AM exposures for patientsor =75 years (10.5%) were 19% (90% CI: 1.11-1.28) higher compared with patients75 years.

Published
2009
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18. Population pharmacokinetics and pharmacodynamics of prasugrel and clopidogrel in aspirin-treated patients with stable coronary artery disease

Author

David S. Small, Kenneth J. Winters, Shashank Rohatagi, Rebecca E. Wrishko, Lars Wallentin, Daniel E. Salazar, and C. Steven Ernest

Subjects
Male, Ticlopidine, Prasugrel, Platelet Aggregation, Thienopyridine, Coronary Artery Disease, Thiophenes, Pharmacology, Models, Biological, Loading dose, Drug Administration Schedule, Piperazines, Double-Blind Method, medicine, Humans, Active metabolite, Prasugrel Hydrochloride, Aspirin, Maintenance dose, Chemistry, Middle Aged, Clopidogrel, Pharmacodynamics, Female, Platelet Aggregation Inhibitors, medicine.drug
Abstract

The aim of the current analysis was to characterize the population PK of prasugrel and clopidogrel metabolites, the resulting PD response, and identification of covariates for key PK/PD parameters. Aspirin-treated subjects with coronary artery disease were randomized to double-blind treatment with clopidogrel 600 mg loading dose (LD) followed by daily 75 mg maintenance dose (MD) or prasugrel 60 mg LD and daily 10 mg MD for 28 days. Plasma concentrations of prasugrel active metabolite (Pras-AM) and prasugrel's inactive thiolactone metabolite (Pras-thiolactone) were simultaneously fit to a multicompartmental model; a similar model adequately described clopidogrel's active metabolite (Clop-AM) PK. By linking to the PK model through the active metabolite concentrations, the PK/PD model characterized the irreversible inhibition of platelet aggregation through a sigmoidal Emax model. Although dose, sex, and weight were identified as significant covariates in the prasugrel PK model, only the effect of body weight produced significant changes in Pras-AM exposure. Generally, these factors resulted in only minor changes in Pras-AM exposures such that, overall, the change in the resulting maximal platelet aggregation (MPA) was predicted to be < or =10% points on average. The clopidogrel PK model included dose as a covariate indicating that a significantly less-than-proportional increase in Clop-AM exposure is expected over the dose range of 75-600 mg, thus, the model-predicted PD response is lower than might be anticipated given an 8-fold difference in dose and lower than that typically achieved following prasugrel 60 mg LD. The greater PD response with prasugrel compared with clopidogrel was accounted for by greater conversion of dose to active metabolite.

Published
2008
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19. Pharmacokinetic Interaction Between Tadalafil and Bosentan in Healthy Male Subjects

Author

Rebecca E. Wrishko, Albert Yu, Jasper Dingemanse, Diane L. Phillips, Malcolm I. Mitchell, and Christelle Darstein

Subjects
Pulmonary and Respiratory Medicine, Adult, Male, Metabolic Clearance Rate, Phosphodiesterase Inhibitors, Cmax, Administration, Oral, Pharmacology, Critical Care and Intensive Care Medicine, Tadalafil, Humans, Medicine, Drug Interactions, Pharmacology (medical), CYP2C9, Antihypertensive Agents, Fatigue, Sulfonamides, Cross-Over Studies, Dose-Response Relationship, Drug, CYP3A4, business.industry, Endothelin receptor antagonist, Headache, Bosentan, Middle Aged, Crossover study, respiratory tract diseases, Area Under Curve, cGMP-specific phosphodiesterase type 5, Cardiology and Cardiovascular Medicine, business, Carbolines, medicine.drug
Abstract

Tadalafil, an oral phosphodiesterase 5 (PDE5) inhibitor, is being investigated as a treatment for pulmonary arterial hypertension. Bosentan is an oral endothelin receptor antagonist widely used in the treatment of pulmonary arterial hypertension. Tadalafil is mainly metabolized by cytochrome P450 (CYP) 3A4, and as bosentan induces CYP2C9 and CYP3A4, a pharmacokinetic interaction is possible between these agents. This open-label, randomized study investigated whether any pharmacokinetic interaction exists between tadalafil and bosentan. Healthy adult men (n = 15; 19-52 years of age) received 10 consecutive days of tadalafil 40 mg once daily, bosentan 125 mg twice daily, and a combination of both in a 3-period, crossover design. Following 10 days of multiple-dose coadministration of bosentan and tadalafil, compared with tadalafil alone, tadalafil geometric mean ratios (90% confidence interval [CI]) for AUCtau and Cmax were 0.59 (0.55, 0.62) and 0.73 (0.68, 0.79), respectively, with no observed change in tmax. Following coadministration of bosentan with tadalafil, bosentan ratios (90% CI) for AUCtau and Cmax were 1.13 (1.02, 1.24) and 1.20 (1.05, 1.36), respectively. Tadalafil alone and combined with bosentan was generally well tolerated. In conclusion, after 10 days of coadministration, bosentan decreased tadalafil exposure by 41.5% with minimal and clinically irrelevant differences (

Published
2008
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20. Tadalafil pharmacokinetics in healthy subjects

Author

S. Thomas Forgue, Diane L. Phillips, Beverley Patterson, Malcolm I. Mitchell, Alun Bedding, Christopher D. Payne, and Rebecca E. Wrishko

Subjects
Adult, Male, Adolescent, Metabolic Clearance Rate, Phosphodiesterase Inhibitors, Biological Availability, Pharmacology, Multiple dosing, Drug Administration Schedule, Body Mass Index, Tadalafil, Eating, Pharmacokinetics, Metabolic clearance rate, medicine, Humans, Pharmacology (medical), Aged, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Healthy subjects, Middle Aged, medicine.disease, Crossover study, Circadian Rhythm, Erectile dysfunction, Female, business, Carbolines, Biological availability, medicine.drug
Abstract

To characterize tadalafil plasma pharmacokinetics in healthy subjects following single and multiple doses.Noncompartmental parameters were calculated for healthy subjects receiving a single 2.5-20-mg tadalafil dose in 13 clinical pharmacology studies. An integrated statistical analysis of results in 237 subjects provided global averages and an assessment of effects of body mass index (BMI), age, gender and smoking status. Diurnal variation, food effects and proportionality of exposure to dose were analysed in three studies. Multiple-dose pharmacokinetics were evaluated in a separate study in which parallel groups of 15 subjects received 10 or 20 mg tadalafil once daily for 10 days.Tadalafil was absorbed rapidly with mean Cmax (378 microg l-1 for 20 mg) observed at 2 h; thereafter, concentrations declined nearly monoexponentially with a mean (5th, 95th percentiles) t1/2 of 17.5 (11.5, 29.6) hours. Mean oral clearance (CL/F) was 2.48 (1.35, 4.35) l h-1 and apparent volume of distribution (Vz/F) was 62.6 (39.5, 92.1) l. No clinically meaningful effect of BMI, age, gender or smoking was identified. Exposure was not substantially affected by time of dosing. Food had negligible effects on bioavailability as assessed by 90% confidence intervals for Cmax and AUC mean ratios. Parameters were proportional to dose, indicating that doubling the dose doubled exposure. Steady state was attained by day 5 following once-daily administration, and accumulation (1.6-fold) was consistent with the t1/2.Tadalafil pharmacokinetics are linear with respect to dose and time, and are not affected by food. Systemic clearance is low relative to other phosphodiesterase 5 inhibitors.

Published
2006
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21. Inhibition of Mycelial Growth by Methotrexate in Neurospora crassa Wild Type and Mutants Deficient in Folylpolyglutamate Synthase

Author

Rebecca E. Wrishko and Edwin A. Cossins

Subjects
Crystallography, biology, Clinical Biochemistry, Mutant, Folylpolyglutamate synthase, Wild type, met-6 mutants, biology.organism_classification, Biochemistry, mtx polyglutamates, Neurospora crassa, fpgs-deficient mutants, QD901-999, medicine, Molecular Medicine, Methotrexate, mac mutants, Mycelium, neurospora crassa, medicine.drug
Abstract

Summary In mammalian cells, folylpolyglutamate synthase (FPGS) catalyzes the polyglutamylation of methotrexate (MTX), a reaction that significantly enhances the cellular retention and cytotoxicity of this antifolate. In contrast, MTX is a poor substrate for the cytosolic FPGS of Neurospora crassa. The present study has therefore examined the effect of MTX on growth of N. crassa wild type (FGSC 853 ) and two mutants (met-6, FGSC 1330 and mac, FGSC 3609) that have lesions affecting FPGS expression. Mycelial dry weights after growth in MTX-supplemented media, suggested that met-6 and mac were more sensitive to the antifolate than the wild type (WT). MTX concentrations resulting in 50% inhibition of growth (ICso values) were 5.5 11M, 6.0 11M and 87.5 11M for met-6, mac, and WT, respectively. When MTX treatment was followed by transfer to 50 11M folinic acid-supplemented media, growth of both mutants was enhanced by ca. 20% while that of WT increased by ca. 8%. [3H]-MTX pulse-chase experiments demonstrated that all three strains had limited or no ability to form polyglutamates (MTXGlun ) of the antifolate. In WT cultures, supplied with 1 I-tM [3H]-MTX for 24 hr and then grown in MTX-free media for another 24 hr, over 95% of the recovered label was in MTX; MTXGlu2 and MTXGlu3 accounting for only 2% and 1% respectively. MTXGlun derivatives were not detected in mac but low levels of MTXGlu2 were generated by met-6. In all three strains, the level of expression of dihydrofolate reductase (DHFR) was similar. DHFR was purified to apparent homogeneity (21.6 kDa) from extracts of each strain using a protocol of ammonium sulfate fractionation, gel filtration and Matrex Green A chromatography. It is concluded that in Neurospora, MTX polyglutamylation is not a major factor in the cytotoxicity of this antifolate.

Published
1998

22. A Pharmacokinetic Study of Cyclosporin (Sandimmune??)

Author

Dennis R. N. Primmett, Rebecca E. Wrishko, Marc Levine, and Paul Keown

Subjects
business.industry, Significant difference, General Medicine, Absorption (skin), Elimination kinetics, Pharmacology, Trough (economics), Dosage form, Pharmacokinetics, Renal transplant, Medicine, Pharmacology (medical), Trough Concentration, business
Abstract

In this study, we have investigated the absorption and elimination kinetics of cyclosporin (CsA) at once-daily and twice-daily (at 0800h and 2000h) dosage intervals from the 2 earlier dosage forms, Sandimmune® Oral Solution (OS) and Sandimmune® Soft Gel Capsules (SGC), in 11 stable renal transplant patients. Our objective was to illustrate and explain the factors that are responsible for the poor performance of trough levels in the prediction of CsA exposure and to show how these problems may be overcome in the future by the administration of a new dosage form of CSA, Sandimmune Neoral® (Neoral®). Predose trough levels for OS and SGC in the 0800- and 2000-hour intervals, and for SGC in the once-daily interval, were not significantly different. In the 0800-hour interval, the time to maximum drug concentration for the OS dosage form was significantly longer than for SGC. Analysis of the data from all patients showed no significant difference in dose-adjusted area under the concentration-time curve from zero to 12 hours (AUC0–12h) between 0800-hour and once-daily intervals; however, those results were affected by high intrasubject variability in absorption rate exhibited by a few individuals. Analysis of the data from 7 individuals with very uniform blood CsA concentration profiles revealed a significant dose-dependent effect on CsA absorption. Diurnal fluctuations in SGC absorption rate and extent had significant effects on postdose trough levels: in the 2000-hour interval, postdose trough concentration (Cmin12) was significantly higher than predose trough concentration (Cmin0). This change reflected both delays in absorption as well as increases in absorption extent. The assessment of the predictive potential of CsA trough levels from SGC 12- (0800-hour) and 24-hour (once-daily) intervals revealed poor correlations between: (1) dose vs AUC0–12h (r = 0.17) and AUC0–24h (r = 0.21), (2) dose vs pre- and postdose 12-hour trough concentrations (r < 0.2 in all cases), and (3) AUC0–12h vs predose (r = 0.16) and postdose (r = 0.49) 12-hour trough concentrations. Better correlations were observed with AUC0–24h vs 24-hour predose (r = 0.85) and postdose (r = 0.88) trough concentrations. The results in this study thus serve to illustrate the complexity underlying the use of predose trough concentrations to either predict the AUC, or calculate a dose, for a subsequent dosage interval.

Published
1997
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23. Prasugrel pharmacokinetics and pharmacodynamics in subjects with moderate renal impairment and end-stage renal disease

Author

John T. Brandt, Rebecca E. Wrishko, David S. Small, Daniel E. Salazar, K. A. Kles, Nagy A. Farid, Ying G. Li, Lan Ni, A. G. Borel, Kenneth J. Winters, Christopher D. Payne, and C. S. Ernest

Subjects
Adult, Male, medicine.medical_specialty, Prasugrel, Thienopyridine, Cmax, Urology, Thiophenes, urologic and male genital diseases, Piperazines, Nephropathy, End stage renal disease, Pharmacokinetics, Internal medicine, medicine, Humans, Pharmacology (medical), Pharmacology, business.industry, Middle Aged, medicine.disease, Endocrinology, Pharmacodynamics, Kidney Failure, Chronic, Female, Kidney Diseases, business, Prasugrel Hydrochloride, Platelet Aggregation Inhibitors, medicine.drug, Kidney disease, Protein Binding
Abstract

Objective: The pharmacokinetic (PK) and pharmacodynamic (PD) responses to prasugrel were compared in three studies of healthy subjects vs. those with moderate or end-stage renal impairment. Methods: Two of the three protocols were parallel-design, open-label, single dose (60-mg prasugrel) studies in subjects with end-stage renal disease (ESRD; n = 12) or moderate renal impairment (n = 10) and matched healthy subjects with normal renal function (n = 10). The third protocol was an open-label, single-dose escalation (5, 10, 30 and 60 mg prasugrel) study in subjects with ESRD (n = 16) and matched healthy subjects with normal renal function (n = 16). Plasma concentrations of prasugrel’s active metabolite were determined and pharmacokinetic parameter estimates were derived. Maximum platelet aggregation (MPA) was measured by light transmission aggregometry using 20 μm adenosine diphosphate as agonist. Results: Across all studies, prasugrel’s Cmax and AUC0–t were 51% and 42% lower in subjects with ESRD than in healthy subjects. AUC0–t did not differ between healthy subjects and subjects with moderate renal impairment. The magnitude of change and time-course profiles of MPA was similar for healthy subjects compared with subjects with moderate renal impairment and those with ESRD. Prasugrel was well-tolerated in all subjects. Conclusion: There was no difference in pharmacokinetics or PD responses between subjects with moderate renal impairment and healthy subjects. Despite significantly lower exposure to prasugrel’s active metabolite in subjects with ESRD, MPA did not differ between healthy subjects and those with ESRD.

Published
2009

24. Effect of age on the pharmacokinetics and pharmacodynamics of prasugrel during multiple dosing: an open-label, single-sequence, clinical trial

Author

Kenneth J. Winters, David S. Small, Nagy A. Farid, Christopher D. Payne, Ying G. Li, Lan Ni, Daniel E. Salazar, C. Steven Ernest, and Rebecca E. Wrishko

Subjects
Adult, Male, Acute coronary syndrome, medicine.medical_specialty, Aging, Prasugrel, Bleeding Time, Platelet Aggregation, medicine.medical_treatment, Analgesic, Population, Thiophenes, Piperazines, Statistics, Nonparametric, Body Mass Index, Young Adult, Pharmacotherapy, Pharmacokinetics, Internal medicine, medicine, Confidence Intervals, Purinergic P2 Receptor Antagonists, Humans, Pharmacology (medical), Prodrugs, Least-Squares Analysis, education, Aged, Aged, 80 and over, education.field_of_study, Aspirin, business.industry, Percutaneous coronary intervention, Fasting, medicine.disease, Surgery, Clinical trial, Adenosine Diphosphate, Drug Therapy, Combination, Female, Tablets, Enteric-Coated, Geriatrics and Gerontology, business, Prasugrel Hydrochloride, Platelet Aggregation Inhibitors, medicine.drug
Abstract

A substantial portion of patients at risk for acute coronary syndrome (ACS) are65 years old. Prasugrel is a novel antiplatelet agent approved for the treatment of ACS patients undergoing percutaneous coronary intervention, and will be used in this population.This study assessed the effect of ageor=65 years on the pharmacokinetics (PK) and pharmacodynamics (PD) of the active metabolite (R-138727) of prasugrel in healthy subjects taking aspirin (acetylsalicylic acid).This was an open-label, single-sequence trial conducted in a single clinical research centre in the UK. A total of 17 subjects aged 65-80 years and 15 subjects aged 20-39 years received a prasugrel 5-mg once-daily maintenance dose for 10 days followed by 10-mg once daily maintenance doses for 10 days. All subjects also received aspirin 75 mg daily. Serial blood samples were collected pre-dose and at various times post-dose for measurement of the active metabolite of prasugrel in plasma on days 10 and 20, following the last 5- and 10-mg prasugrel dose, respectively. PK parameters of the active metabolite of prasugrel included area under the plasma concentration-time curve (AUC) from time zero to the time of the last quantifiable concentration (AUC(last)), maximum plasma concentration (C(max)) and time to C(max) (t(max)). Maximal platelet aggregation (MPA), assessed by light transmission aggregometry using adenosine diphosphate (ADP) 20 micromol/L, was assessed at baseline and on day 10 (5-mg maintenance dose) and day 20 (10-mg maintenance dose). Bleeding times (BTs) were determined on days -5, 1, 10, 11, 20 and 21 using a modified Ivy technique.AUC(last) did not differ significantly between age groups. The steady-state trough MPA to ADP 20 micromol/L during 10-mg maintenance dosing was 30.6% and 26.6% in elderly and young subjects, respectively. Mean MPA was consistently higher in elderly subjects compared with young subjects; however, differences were generally less than ten percentage points. BTs did not differ between the two populations during 5-mg maintenance dosing; however, during 10-mg maintenance dosing, BTs were up to 67% longer in young compared with elderly subjects. A higher frequency of minor bleeding during 10-mg maintenance dosing was observed in elderly subjects compared with young subjects.These data indicate that prasugrel PK and MPA were similar in healthy subjects regardless of age. Compared with younger subjects, elderly subjects had shorter BTs but a greater frequency of mild bleeding-related adverse events.

Published
2009

25. Prediction of prasugrel active metabolite concentrations from 2 downstream inactive metabolite concentrations using multilinear regression analysis

Author

Michael Heathman, Rebecca E. Wrishko, and C. Steven Ernest

Subjects
Adult, Male, Prasugrel, Thienopyridine, Adolescent, Metabolite, Thiophenes, Pharmacology, Models, Biological, Piperazines, chemistry.chemical_compound, Young Adult, Pharmacokinetics, medicine, Humans, Pharmacology (medical), Prodrugs, Active metabolite, Aged, Dose-Response Relationship, Drug, Prodrug, Middle Aged, Adenosine diphosphate, chemistry, Clinical Trials, Phase III as Topic, Linear Models, Platelet aggregation inhibitor, Female, Prasugrel Hydrochloride, Platelet Aggregation Inhibitors, medicine.drug
Abstract

Prasugrel is a thienopyridine prodrug that is metabolized to an active metabolite (Pras-AM), which inhibits adenosine diphosphate (ADP)-induced platelet aggregation. The study objective was to describe a multilinear regression correlation model that was used to quantitatively predict concentrations of Pras-AM from downstream inactive metabolites, R-119251 and R-106583, for the purpose of estimating Pras-AM exposure in patients in the TRITON-TIMI 38 substudies. The model development included 1462 Pras-AM, 1345 R-119251, and 1456 R-106583 concentration data points from 103 healthy participants with a prasugrel dose range of 15 to 80 mg. The model was shown to provide good correlation between predicted and observed concentrations with only a minor deviation of approximately 6% from the unity line and described the variability within approximately 4.5%. Examination of the data indicated that regardless of ethnicity, age, weight, moderate hepatic impairment, or renal impairment, predictions were reliable. Predicted Pras-AM concentrations in TRITON-TIMI 38 were comparable with historical data.

Published
2009

26. Safety, efficacy, and pharmacokinetic overview of low-dose daily administration of tadalafil

Author

David T. Wong, Sebastian Sorsaburu, Rebecca E. Wrishko, James McGill, and Andrew Strawbridge

Subjects
Adult, Male, Time Factors, Phosphodiesterase Inhibitors, Urology, Endocrinology, Diabetes and Metabolism, Pharmacology, law.invention, Tadalafil, Endocrinology, Pharmacokinetics, Randomized controlled trial, Double-Blind Method, Erectile Dysfunction, law, medicine, Health Status Indicators, Humans, Dosing, Aged, Aged, 80 and over, business.industry, Middle Aged, medicine.disease, Clinical trial, Psychiatry and Mental health, Erectile dysfunction, Reproductive Medicine, cGMP-specific phosphodiesterase type 5, Pharmacodynamics, Area Under Curve, business, medicine.drug, Carbolines
Abstract

Introduction Several phosphodiesterase type 5 (PDE5) inhibitors are commercially available for the treatment of erectile dysfunction (ED). Development of the first once-daily alternative dosing regimen with a PDE5 inhibitor was motivated by the behavioral complexities associated with sexual intimacy. Aim To provide an alternative dosing option for certain men who may benefit from the removal of the temporal linkage between administration of an ED therapy and sexual intimacy or for men and their partners who anticipate at least twice-weekly sexual activity. Methods Pharmacokinetic predictions of tadalafil plasma concentrations were generated based upon empirical data following 20-mg, single-dose administration coupled with tadalafil usage patterns from as-needed clinical trials. To support the pharmacokinetic simulations and pharmacodynamic assumptions, clinical trials were conducted to demonstrate the efficacy and safety of once-daily, low-dose tadalafil 2.5 and 5 mg. Main Outcome Measures Simulated tadalafil plasma concentrations and comparison with safety and efficacy measures from clinical trials. Results Based upon pharmacodynamic and pharmacokinetic data, once-daily doses of tadalafil 5 mg were predicted to provide therapeutic concentrations that would be maintained throughout the 24-hour dosing interval. Additionally, for a subgroup of men who anticipate at least twice-weekly sexual activity and are currently taking tadalafil 20 mg, a reduction in daily tadalafil exposure was predicted. To support the hypothesis that low-dose, once-daily tadalafil may be a safe and effective treatment alternative, clinical trials were conducted to demonstrate the safety and efficacy of once-daily tadalafil 2.5 and 5 mg. These results were similar to those of historical as-needed studies evaluating tadalafil 10 and 20 mg. Conclusions Consistent with pharmacokinetic predictions, data from clinical trials indicate that once-daily use of low-dose tadalafil is a safe and effective treatment for men with ED. Wrishko R, Sorsaburu S, Wong D, Strawbridge A, and McGill J. Safety, efficacy, and pharmacokinetic overview of low-dose daily administration of tadalafil. J Sex Med 2009;6:2039–2048.

Published
2009

27. Abstract 4001: Relationship between Exposure to the Prasugrel Active Metabolite with TIMI Major/Minor Bleeding in TRITON-TIMI 38

Author

Daniel E Salazar, C. Steven Ernest, Rebecca E Wrishko, Govinda J Weerakkody, David S Small, Ying G Li, Shashank Rhohatagi, Bruce E Dornseif, Lan Ni, Elliot M Antman, Stephen D Wiviott, William L Macias, and Jeffrey S Riesmeyer

Subjects
Physiology (medical), Cardiology and Cardiovascular Medicine
Abstract

In TRITON-TIMI 38, patients treated with prasugrel had a higher incidence of TIMI bleeding compared to treatment with clopidogrel. Increased bleeding was most evident in patients

Published
2008
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28. CYP2D6 metabolizer status and atomoxetine dosing in children and adolescents with ADHD

Author

Jennifer Witcher, Peter D. Feldman, David W. Williams, Paula T. Trzepacz, Rebecca E. Wrishko, and Jan K. Buitelaar

Subjects
Male, CYP2D6, medicine.medical_specialty, Time Factors, 110 012 Social cognition of verbal communication, Adolescent, Neuroinformatics [DCN 3], Atomoxetine Hydrochloride, QT interval, Mental health [NCEBP 9], 150 000 MR Techniques in Brain Function, Cognitive neurosciences [UMCN 3.2], Weight loss, Internal medicine, medicine, Perception and Action [DCN 1], Determinants in Health and Disease [EBP 1], Humans, Attention deficit hyperactivity disorder, Pharmacology (medical), Dosing, Child, Biological Psychiatry, Pharmacology, Adrenergic Uptake Inhibitors, Dose-Response Relationship, Drug, Propylamines, Hepatic cytochrome, Atomoxetine, medicine.disease, Psychiatry and Mental health, Cytochrome P-450 CYP2D6, Neurology, Tolerability, Attention Deficit Disorder with Hyperactivity, Anesthesia, Drug Evaluation, Female, Neurology (clinical), medicine.symptom, Psychology, medicine.drug
Abstract

Contains fulltext : 70123.pdf (Publisher’s version ) (Closed access) To determine whether physicians can adequately titrate atomoxetine without knowing genotype status for hepatic cytochrome P450 2D6, we pooled data from two open-label studies of atomoxetine in children and adolescents with attention-deficit/hyperactivity disorder. Patients were assessed weekly up to 10 weeks and doses titrated for efficacy and tolerability at the discretion of investigators (max. 1.8 mg/kg/d). Mean dose was 0.1 mg/kg/d lower in poor metabolizer (PM) patients (n=87) than extensive metabolizers (EMs, n=1239). PMs demonstrated marginally better efficacy on the ADHDRS-IV-Parent:Inv and had comparable safety profiles, except for a 4.0-bpm greater increase in mean pulse rate and a 1.0-kg greater weight loss. Changes from baseline in Fridericia QTc did not differ between groups or correlate with dose in PMs. Results suggest genotyping is unnecessary during routine clinical management, because investigators were able to dose atomoxetine to comparable efficacy and safety levels in EMs and PMs without knowledge of genotype metabolizer status.

Published
2008

29. Effects of gender, age, diabetes mellitus and renal and hepatic impairment on tadalafil pharmacokinetics

Author

Rebecca E. Wrishko, Christopher D. Payne, Alun Bedding, Hayley Jewell, S. Thomas Forgue, Diane L. Phillips, Malcolm I. Mitchell, and Beverley Patterson

Subjects
Adult, Male, medicine.medical_specialty, Phosphodiesterase Inhibitors, Nephropathy, Tadalafil, Sex Factors, Pharmacokinetics, Belgium, Erectile Dysfunction, Internal medicine, Diabetes mellitus, Germany, medicine, Diabetes Mellitus, Humans, Pharmacology (medical), Pharmacology, business.industry, Hepatic impairment, Liver Diseases, Age Factors, Middle Aged, medicine.disease, United Kingdom, Surgery, Erectile dysfunction, Research centre, Female, Kidney Diseases, Poland, business, medicine.drug, Kidney disease, Carbolines
Abstract

To evaluate the effects of gender, age, diabetes mellitus, renal and hepatic impairment on tadalafil pharmacokinetics and tolerability.Six single-dose (5, 10 or 20 mg orally) clinical pharmacology studies were conducted in the UK, Belgium, Poland and Germany in healthy male and female subjects, elderly subjects and subjects with diabetes mellitus, renal impairment, end-stage renal failure (ESRF) or hepatic impairment. The gender study also incorporated administration of 10 mg tadalafil daily for 10 days.Systemic exposure in the elderly was 25% greater than in young subjects (mean AUC ratio 1.25; 90% confidence interval 0.972, 1.61). The AUC was 19% lower in subjects with diabetes mellitus than in healthy age/gender-matched controls. Pharmacokinetics in female subjects were essentially similar to those in males. Exposure in subjects with mild or moderate renal insufficiency was approximately twice that in healthy subjects. The mean AUC for the major metabolite (total methylcatechol glucuronide) in the presence of ESRF was three times the mean for healthy subjects. Haemodialysis contributed negligibly to elimination of tadalafil or the metabolite. Hepatic impairment had negligible effects on exposure. The most common adverse events in these six studies were headache, back pain and myalgia. A 10-mg dose was not well tolerated by subjects with moderate renal dysfunction in this study.No clinically significant effect of gender, age, diabetes mellitus or hepatic impairment on tadalafil pharmacokinetics was observed. Renal insufficiency resulted in increased systemic exposure. Tadalafil was not associated with any serious clinically significant adverse events or study discontinuations due to adverse events.

Published
2006

30. Vancomycin pharmacokinetics and Bayesian estimation in pediatric patients

Author

Phyllis Abbott, Rebecca E. Wrishko, Dominique Khoo, Don Hamilton, and Marc S. Levine

Subjects
Male, medicine.medical_specialty, Population, Urology, Cohort Studies, Bayes' theorem, Pharmacokinetics, Vancomycin, medicine, Humans, Pharmacology (medical), education, Child, Antibacterial agent, Pharmacology, Bayes estimator, education.field_of_study, medicine.diagnostic_test, business.industry, Bayes Theorem, NONMEM, Anti-Bacterial Agents, Therapeutic drug monitoring, Anesthesia, Child, Preschool, Female, Drug Monitoring, business, medicine.drug
Abstract

The vancomycin pharmacokinetic profile was characterized in six pediatric patients and the potential of nonlinear mixed effects modeling and Bayesian forecasting for vancomycin monitoring was explored using NONMEM V (1.1). Based on steady state serial vancomycin concentrations, the estimates of mean t1/2, Vd, and Cl derived by the Sawchuk and Zaske method (1) were 3.52 hours, 0.57 L/kg, and 0.12 L/h per kg, respectively. NONMEM analysis demonstrated that a weight-adjusted two-compartment model described individual patients' data better than a comparable one-compartment model. The two-compartment estimates of mean t1/2alpha, t1/2beta, Vss, and Cl were 0.80 hour, 5.63 hours, 0.63 L/kg, and 0.11 L/h per kg, respectively. The relatively long mean t1/2alpha suggests that peak vancomycin concentrations measured earlier than 4 hours postdose do not reflect postdistributional serum concentrations. NONMEM population modeling revealed that a weight-adjusted two-compartment model provided a better fit than a comparable one-compartment model. The resulting population parameters and variances were fixed in NONMEM to obtain Bayesian predictions of individual vancomycin serum concentrations. Bayesian estimation with either a single midinterval or trough sample has the potential to provide accurate and precise predictions of vancomycin concentrations. This should be evaluated using a vancomycin population pharmacokinetic model based on a larger sample of pediatric patients.

Published
2000

31. Investigation of a possible interaction between ciprofloxacin and cyclosporine in renal transplant patients

Author

Nilufar Partovi, Marc S. Levine, Stevan Lewis, Dennis R. N. Primmett, Susan Kim, Rebecca E. Wrishko, Paul Keown, and David Landsberg

Subjects
Graft Rejection, Male, Reoperation, medicine.medical_specialty, medicine.medical_treatment, Biopsy, Gastroenterology, Anti-Infective Agents, Ciprofloxacin, Internal medicine, medicine, Humans, Drug Interactions, Retrospective Studies, Transplantation, Chemotherapy, Kidney, Chi-Square Distribution, business.industry, Incidence (epidemiology), Drug interaction, Middle Aged, Ciclosporin, Kidney Transplantation, Surgery, medicine.anatomical_structure, Case-Control Studies, Cyclosporine, Female, business, Complication, Immunosuppressive Agents, medicine.drug
Abstract

Background. Bacterial infection is a common complication during the first few months after renal transplantation. Ciprofloxacin, a fluoroquinolone broad-spectrum antibiotic, is used frequently in treating infections in the early posttransplant period. Evidence from in vitro studies has suggested that ciprofloxacin can antagonize the cyclosporine (CsA)-dependent inhibition of interleukin-2 production. Such an effect in renal transplant patients could antagonize the immunosuppressive activity of CsA and lead to rejection of the graft. Methods. To investigate the possibility of a pharmacodynamic interaction between ciprofloxacin and CsA, we conducted a case-control study in 42 patients who had received a kidney transplant and who were prescribed ciprofloxacin in the first 1-6 months after transplantation and in their matched controls (two per case) who did not receive ciprofloxacin during the study period. Results. There was a twofold greater incidence (P=0.008) of ciprofloxacin use at 1-3 months (65%) than was observed at 4-7 months (35%) after transplantation. The proportion of cases experiencing at least one episode of biopsy-proven rejection 1-3 months posttransplant (45%) was significantly greater (P=0.004) than that of controls (19%). Furthermore, there was a marked increase (P

Published
1997

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