Your search keyword '"Pappas F"' showing total 4 results

1. Characterizing Absorption Properties of Dispersible Pretomanid Tablets Using Population Pharmacokinetic Modelling

Author

Zou, Y., Nedelman, J., Lombardi, A., Pappas, F., Karlsson, M.O., Svensson, E.M., Zou, Y., Nedelman, J., Lombardi, A., Pappas, F., Karlsson, M.O., and Svensson, E.M.

Abstract

Item does not contain fulltext, BACKGROUND AND INTRODUCTION: The dispersible tablet formulation (DTF) of pretomanid has been developed to facilitate future use in children. This work aimed to assess the pharmacokinetics (PK) and relative bioavailability of the DTF compared to the marketed formulation (MF) and the potential influence of dose. METHODS: Pretomanid DTF was investigated in a single-dose, randomized, four-period, cross-over study, with 7 days of washout between doses. Forty-eight healthy volunteers were enrolled and randomized into one of two panels to receive doses either in the fasted state or after a high-fat meal. Each volunteer received doses of 10, 50, and 200 mg DTF, and 200 mg MF pretomanid. Blood samples for pharmacokinetic assessment were drawn following a rich schedule up to 96 h after each single dose. The study data from the panel receiving the high-fat meal were analyzed using a nonlinear mixed-effects modeling approach, and all data were characterized with noncompartmental methods. RESULTS: A one-compartment model with first-order elimination and absorption through a transit compartment captured the mean and variability of the observed pretomanid concentrations with acceptable precision. No significant difference in bioavailability was found between formulations. The mean absorption time for the DTF was typically 137% (86-171%) of that for the MF. The bioavailability was found to be dose dependent with a small positive and larger negative correlation under fed and fasted conditions, respectively. CONCLUSION: Using data from a relative bioavailability study in healthy adult volunteers, a mathematical model has been developed to inform dose selection for the investigation of pretomanid in children using the new dispersible tablet formulation. Under fed conditions and at the currently marketed adult dose of 200 mg, the formulation type was found to influence the absorption rate, but not the bioavailability. The bioavailability of the DTF was slightly positively correlated wi

Published

2022

2. Characterizing Absorption Properties of Dispersible Pretomanid Tablets Using Population Pharmacokinetic Modelling

Author

Zou, Y., Nedelman, J., Lombardi, A., Pappas, F., Karlsson, M.O., Svensson, E.M., Zou, Y., Nedelman, J., Lombardi, A., Pappas, F., Karlsson, M.O., and Svensson, E.M.

Abstract

Contains fulltext : 287863.pdf (Publisher’s version ) (Open Access), BACKGROUND AND INTRODUCTION: The dispersible tablet formulation (DTF) of pretomanid has been developed to facilitate future use in children. This work aimed to assess the pharmacokinetics (PK) and relative bioavailability of the DTF compared to the marketed formulation (MF) and the potential influence of dose. METHODS: Pretomanid DTF was investigated in a single-dose, randomized, four-period, cross-over study, with 7 days of washout between doses. Forty-eight healthy volunteers were enrolled and randomized into one of two panels to receive doses either in the fasted state or after a high-fat meal. Each volunteer received doses of 10, 50, and 200 mg DTF, and 200 mg MF pretomanid. Blood samples for pharmacokinetic assessment were drawn following a rich schedule up to 96 h after each single dose. The study data from the panel receiving the high-fat meal were analyzed using a nonlinear mixed-effects modeling approach, and all data were characterized with noncompartmental methods. RESULTS: A one-compartment model with first-order elimination and absorption through a transit compartment captured the mean and variability of the observed pretomanid concentrations with acceptable precision. No significant difference in bioavailability was found between formulations. The mean absorption time for the DTF was typically 137% (86-171%) of that for the MF. The bioavailability was found to be dose dependent with a small positive and larger negative correlation under fed and fasted conditions, respectively. CONCLUSION: Using data from a relative bioavailability study in healthy adult volunteers, a mathematical model has been developed to inform dose selection for the investigation of pretomanid in children using the new dispersible tablet formulation. Under fed conditions and at the currently marketed adult dose of 200 mg, the formulation type was found to influence the absorption rate, but not the bioavailability. The bioavailability of the DTF was slightly positively correlated wi

Published

2022

3. Improving physical properties of rubber compounds containing devulcanized rubber

Author

Pappas F., e-Rubbercon 2020, Association Francaise des Ingenieurs et Cadres du Caoutchouc et des Polymeres (AFICEP), Paris, France, 11-12/02/2021, Pappas F., e-Rubbercon 2020, Association Francaise des Ingenieurs et Cadres du Caoutchouc et des Polymeres (AFICEP), Paris, France, and 11-12/02/2021

Published

2021

4. Ada (trade name) Portability Guidelines.

Author

SOFTECH INC WALTHAM MA, Pappas,F., SOFTECH INC WALTHAM MA, and Pappas,F.

Abstract

This report presents the results of a study in using Ada to write portable programs. These programs with little or no modification, can be used in different target environments than those for which they were originally written. Ordinarily, a different target environment means a different computer, although the difference may instead be in the target operating system or peripherals. Software portability is one of the main cost-saving benefits anticipates with the use of Ada. Support for portability was a major goal in the design of the Ada language. However, portability does not come automatically with the use of Ada; programs written without specific attention to portability will not in general be portable. This report presents guidelines to be followed in order to produce code that is portable. A major goal in undertaking this study was support for development of a highly-portable Ada implementation of the JINTACCS Automated Message Preparation System (JAMPS). However, the guidelines are equally applicable to any program requiring portability. The guidelines are designed to permit an office conducting an acquisition to supply them to contractors as direction or guidance . They may also be useful in evaluating the portability of an existing implementation.

Published

1985