Zobrazeno 1 - 10
of 43
pro vyhledávání: '"Geraldine M, Ferron"'
Autor:
Jean-Louis Pinquier, Frank A. S. Erwich, Sandrine Turpault, Franck Poitiers, Christine Roy, Linda E. Klumpers, Geraldine M. Ferron, Johan G. C. van Hasselt, Lineke Zuurman, Joop M. A. van Gerven
Publikováno v:
British Journal of Clinical Pharmacology. 76:65-77
Aim Cannabinoid receptor type 1 (CB1) antagonists have been developed for the treatment of obesity and associated risk factors. Surinabant is a high affinity CB1 antagonist in vitro. The aim of this study was to assess the magnitude of inhibition by
Publikováno v:
British Journal of Clinical Pharmacology. 56:39-45
Aims To evaluate potential pharmacokinetic interactions between phenobarbitone and retigabine, a new antiepileptic drug. Methods Fifteen healthy men received 200 mg of retigabine on day 1. On days 4–32, phenobarbitone 90 mg was administered at 22.0
Autor:
Geraldine M. Ferron, JoAnn Scatina, Simon E. Ball, Qian Xiang, Lilian G. Yengi, John Kao, C. Roland Wolf, Richard Fruncillo, Jinmei Pan
Publikováno v:
Analytical Biochemistry. 316:103-110
There is considerable interindividual variation in man’s ability to metabolize drugs and foreign compounds. These differences can partly be attributed to genetic polymorphisms that result in the generation of multiple phenotypes with different drug
Autor:
Jeffrey Paul, Norbert G. Knebel, Katharina Erb, Lyette S Richards, Hans‐Peter Cnota, Robert Hermann, Geraldine M. Ferron, Peter Ruus, Steven M. Troy
Publikováno v:
Clinical Pharmacology & Therapeutics. 73:61-70
Background The novel antiepileptic drug retigabine is the first selective M-current potassium channel opener for KCNQ2/3 and KCNQ3/5 channels. Retigabine undergoes phase II metabolism (N-glucuronidation, acetylation) exclusively and renal excretion.
Autor:
Geraldine M. Ferron, Jeffrey Paul, Paul J. Pockros, Richard A. Preston, Marybeth Turner, John Getsy, Robert J. Noveck, Madelyn Abell, Philip R. Mayer
Publikováno v:
Clinical Therapeutics. 23:1180-1192
Background: Patients with impaired hepatic function usually require gastric acid—suppressant therapy but are at increased risk for drug interactions and may require dosage adjustments. The proton pump inhibitor pantoprazole is rapidly absorbed and
Publikováno v:
The Journal of Clinical Pharmacology. 41:149-156
The relationship between the pharmacokinetics of pantoprazole, an irreversible proton pump inhibitor, and its effect on gastric acid secretion was evaluated in humans and rats. Pantoprazole pharmacokinetics were studied in 6 rats (5 mg/kg, i.v.) and
Publikováno v:
The Journal of Clinical Pharmacology. 39:1155-1161
The bioavailability of an oral nonaqueous solution of sirolimus was compared under fasting conditions and after a high-fat meal in a randomized, two-way crossover pharmacokinetic study. Healthy volunteers were administered a 15 mg single dose of siro
Publikováno v:
Journal of Pharmacokinetics and Biopharmaceutics. 27:1-21
Prednisolone (Pred) and sirolimus (SIR) are immunosuppressive compounds acting through different mechanisms with moderate synergism found in vitro. Both drugs are metabolized partly by CYP3A enzymes. After iv administration of placebo, Pred (5 mg/kg)
Publikováno v:
Transplantation. 65:1203-1209
The immunologic response is one barrier to successful transplantation and T cell-mediated rejection is the major contributor to acute and chronic rejections leading to graft failure (1). Thus, to avoid or delay rejection, inimunosuppressive therapy i
Autor:
Geraldine M. Ferron, William J. Jusko
Publikováno v:
Pharmaceutical Research. 15:1888-1894
Purpose. To assess pharmacokinetic and pharmacoimmunodynamic interactions between prednisolone (Pred, 1 mg/kg) and sirolimus (Sir, 0.25 mg/kg) in rabbits.