Your search keyword '"S. Troy"' showing total 12 results

1. Carry‐over effects of nestling physical condition predict first‐year survival of a critically endangered migratory parrot

Author

L. T. Bussolini, R. Crates, A. Herrod, M. J. L. Magrath, S. Troy, and D. Stojanovic

Subjects

Ecology, Nature and Landscape Conservation

Published

2023

2. Regulation of Emotions Under Stress

Author

Amanda J. Shallcross, Iris B. Mauss, and Allison S. Troy

Subjects

medicine.medical_specialty, media_common.quotation_subject, Public health, Physical health, Cognitive reappraisal, Extant taxon, Stress (linguistics), medicine, Psychological resilience, Empirical evidence, Psychology, Social psychology, Physical illness, media_common

Abstract

Stressful life events (SLEs) are frequently associated with a range of deleterious mental and physical health outcomes. However, some individuals exhibit resilience, defined as maintained or even improved health in the wake of SLEs. How and why might this be the case? Given that SLEs give rise to negative emotions, which in turn contribute to mental and physical illness, promising answers to questions about resilience lie in research on people's ability to manage their emotions, or, emotion regulation. This essay focuses on emerging empirical evidence that suggests that two seemingly opposite emotion regulation strategies, cognitive reappraisal and emotional acceptance, are particularly effective for managing negative emotions, which, in turn, may confer resilience. By integrating theory with extant empirical evidence, we offer a model that aims to reconcile how these two strategies—one that involves minimizing emotions (cognitive reappraisal) and the other that involves engaging with emotions (emotional acceptance)—are each associated with resilience. Specifically, we propose that these strategies are not contradictory, but rather complementary. We additionally discuss broader implications for the links among stress, emotion regulation, and health, as well as key issues for future research at the intersection of social and clinical psychology, medicine, and public health. Keywords: stress; emotion regulation; mental and physical health; cognitive reappraisal; acceptance

Published

2015

3. Potentiation of antineoplastic drugs in vitro and in vivo by DNA intercalating bioreductive agents

Author

William D. Bloomer, Michael W. Epperly, Anna Miller, Maria V. Papadopoulou, and B S Troy Seskey

Subjects

Melphalan, Radiation, Radiological and Ultrasound Technology, Chemistry, Glutathione, Pharmacology, In vitro, chemistry.chemical_compound, Oncology, Chemosensitization, In vivo, Toxicity, medicine, Cytotoxic T cell, Radiology, Nuclear Medicine and imaging, Doxorubicin, medicine.drug

Abstract

Three recently synthesized 2-nitroimidazole-linked acridine DNA intercalators (NLA-1, NLA-2, and NLA-4) have been studied as potentiators of the cytotoxic effect of melphalan (L-PAM), 1-(2-chloroethyl)-3-cyclohexyl-1-nitrosourea (CCNU), cis-diamminedichloroplatinum (II) (cis-DDP), and doxorubicin in V79 cells. In vivo studies have also been performed with all three sensitizers and L-PAM, while NLA-1 alone was examined for potentiation of cis-DDP, using C3H/HEJ mice, bearing a murine ovarian tumor. Significant chemosensitization was observed in vitro with L-PAM, CCNU, and cis-DDP after hypoxic preincubation treatment of the cells (37°C) at negligible concentrations of each sensitizer, while inhibition was observed with doxorubicin. Long hypoxic preexposure times at relatively low sensitizer doses were more effective than short hypoxic preexposure times at high sensitizer doses for potentiation. Glutathione depletion studies in vitro with diethyl maleate (DEM) showed that only less than half of the enhanced toxicity observed with NLA-1 or NLA-4 and L-PAM is due to glutathione depletion by the sensitizer. The LD50/35 value in C3H/HEJ mice for NLA-1, NLA-2, and NLA-4 was 45, 25, and 63 mg/kg, respectively. Significant antitumor effect was observed in vivo when 25 mg/kg of NLA-1 was administered i.p. to tumor-bearing mice 2 hr before L-PAM administration (2.5 mg/ kg, i.p.). With this combination pattern of sensitizer:antineoplastic drug, 50% cures were observed in mice followed for >150 days; no long-term survivors were observed with L-PAM therapy alone. © 1993 Wiley-Liss, Inc.

Published

1993

4. A Randomized, Prospective Evaluation of an Interventional Program to Discontinue Intravenous Antibiotics at Two Tertiary Care Teaching Institutions

Author

Bailey, Thomas C., primary, Ritchie, David J., additional, McMullin, S. Troy, additional, Kahn, Michael, additional, Reichley, Richard M., additional, Casabar, Ed, additional, Shannon, William, additional, and Dunagan, William Claiborne, additional

Published

1997

5. THERMAL RESISTANCE OF LACTIC ACID BACTERIA AND YEAST IN ORANGE JUICE AND CONCENTRATE

Author

J. F. Folinazzo, V. S. Troy, and D. I. Murdock

Subjects

Orange juice, chemistry.chemical_compound, biology, Chemistry, Thermal resistance, Food science, biology.organism_classification, Yeast, Bacteria, Food Science, Lactic acid

Published

1953

6. Pharmacokinetic Modeling of Intrathecally Administered Recombinant Human Arylsulfatase A (TAK-611) in Children With Metachromatic Leukodystrophy.

Author

Troy S, Wasilewski M, Beusmans J, and Godfrey CJ

Subjects

Cerebroside-Sulfatase pharmacokinetics, Child, Child, Preschool, Half-Life, Humans, Infant, Injections, Spinal, Tissue Distribution, Brain metabolism, Cerebroside-Sulfatase administration & dosage, Leukodystrophy, Metachromatic drug therapy, Models, Biological

Abstract

Metachromatic leukodystrophy (MLD) is a lysosomal storage disease caused by deficient arylsulfatase A (ASA) activity, which leads to neuronal sulfatide accumulation and motor and cognitive deterioration. Intrathecal delivery of a recombinant human ASA (TAK-611, formerly SHP611) is under development as a potential therapy for MLD. We used serum and cerebrospinal fluid (CSF) TAK-611 concentrations measured during the phase I/II trial of intrathecal TAK-611 to develop a pharmacokinetic (PK) model describing drug disposition. CSF data were well characterized by a two-compartment model in the central nervous system (CNS); a single central compartment described the serum data. Estimated parameters suggested rapid distribution of TAK-611 from CSF into the putative brain tissue compartment, with persistence in the brain between doses (median distributive and terminal half-lives in the CNS: 1.02 and 477 hours, respectively). This model provides a valuable basis for understanding the PK distribution of TAK-611 and for PK/pharmacodynamic analyses of functional outcomes., (© 2019 Shire International GmbH. Clinical Pharmacology & Therapeutics published by Wiley Periodicals, Inc. on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published

2020

7. Effects of age and sex on the disposition of retigabine.

Author

Hermann R, Ferron GM, Erb K, Knebel N, Ruus P, Paul J, Richards L, Cnota HP, and Troy S

Subjects

Adult, Aged, Aged, 80 and over, Anticonvulsants blood, Area Under Curve, Carbamates blood, Creatinine blood, Female, Half-Life, Humans, Male, Phenylenediamines blood, Reference Values, Aging metabolism, Anticonvulsants pharmacokinetics, Carbamates pharmacokinetics, Phenylenediamines pharmacokinetics, Sex Characteristics

Abstract

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., Objective: Our objective was to evaluate the effects of age and sex on the pharmacokinetics of retigabine., Methods: Healthy young (age range, 18-40 years) and elderly (age range, 66-81 years) white subjects (12 men and 12 women in each group) received a single 200-mg oral dose of retigabine. After dosing, blood was collected over a 72-hour period to determine plasma concentrations of retigabine and its acetylated metabolite, AWD21-360. Pharmacokinetics was compared for age group and sex by ANOVA., Results: In young men, retigabine was rapidly absorbed, with the maximum concentration occurring within 2 hours, and was eliminated with an apparent clearance of 0.67 L x h(-1) x kg(-1) and a mean terminal half-life of 8.5 hours. Subjects were similarly exposed to AWD21-360. Compared with young men, young women had higher retigabine maximum concentration (56%) and exposure (20%) but similar clearance (0.68 L x h(-1) x kg(-1)); these differences were related to differences in body weight. Although maximum concentration was similar in elderly subjects, retigabine elimination was slower (30% lower apparent clearance normalized for weight), resulting in higher exposure (42%) and a longer half-life (30%). Because phase II metabolism is scarcely affected by age, these differences may be related to the known decline of renal function with age., Conclusions: Although there are no substantial sex-related differences in the disposition of retigabine, a relevant decrease in clearance resulting in higher exposure occurs in elderly patients. The results suggest that decline of renal function with age may account for some of the observed changes.

Published

2003

8. Multiple-dose, linear, dose-proportional pharmacokinetics of retigabine in healthy volunteers.

Author

Ferron GM, Paul J, Fruncillo R, Richards L, Knebel N, Getsy J, and Troy S

Subjects

Acetylation, Adult, Anticonvulsants administration & dosage, Anticonvulsants adverse effects, Area Under Curve, Biotransformation, Carbamates administration & dosage, Carbamates adverse effects, Chromatography, High Pressure Liquid, Dose-Response Relationship, Drug, Double-Blind Method, Half-Life, Humans, Male, Mass Spectrometry, Phenylenediamines administration & dosage, Phenylenediamines adverse effects, Reproducibility of Results, Anticonvulsants pharmacokinetics, Carbamates pharmacokinetics, Phenylenediamines pharmacokinetics

Abstract

Retigabine, a first-in-class selective M-current potassium channel opener, is a novel antiepileptic compound currently in clinical development. The purpose of this randomized placebo-controlled study was to assess retigabine oral safety and pharmacokinetics in healthy male volunteers (N = 45). Subjects received one dose on day 1 and doses every 12 hours for the next 14 days. Fixed doses were given to the first four groups (200, 400, 500, and 600 mg per day). Titrated doses were given to group 5 in 100 mg increases every 4 days, achieving 700 mg per day on day 15. Serial blood samples were collected on days 1 and 15. Pharmacokinetic parameters were compared between days and among dose groups. After administration of a single dose, retigabine was rapidly absorbed, with maximum concentrations of 387 ng/ml (normalized to a 100 mg dose) occurring within 1.5 hours. Retigabine was eliminated with a mean terminal half-life of 8.0 hours and an apparent oral clearance of 0.70 L/h/kg in white subjects. In black subjects, retigabine clearance and volume of distribution were 25% and 30% lower, respectively, after normalizing by body weight, leading to higher exposure in this population. Retigabine's pharmocokinetics was linearly dose proportional. Steady-state pharmacokinetics was in agreement with single-dose pharmacokinetics, and the accumulation ratio was about 1.5. Retigabine and AWD21-360 trough evening concentrations were significantly lower (about 30% to 35%) than morning values. The titration regimen allowed for higher doses to be tolerated compared to the fixed-dose regimen. In conclusion, the pharmacokinetics of retigabine is linearly dose proportional for daily doses of 100 to 700 mg and is not modified on multiple administrations.

Published

2002

9. Absolute bioavailability and electroencephalographic effects of conventional and extended-release formulations of venlafaxine in healthy subjects.

Author

Patat A, Troy S, Burke J, Trocherie S, Danjou P, Le Coz F, Allain H, and Gandon JM

Subjects

Adult, Area Under Curve, Biological Availability, Cross-Over Studies, Cyclohexanols adverse effects, Cyclohexanols blood, Cyclohexanols pharmacology, Delayed-Action Preparations, Double-Blind Method, Humans, Male, Selective Serotonin Reuptake Inhibitors adverse effects, Selective Serotonin Reuptake Inhibitors blood, Selective Serotonin Reuptake Inhibitors pharmacology, Venlafaxine Hydrochloride, Cyclohexanols pharmacokinetics, Electroencephalography drug effects, Selective Serotonin Reuptake Inhibitors pharmacokinetics

Abstract

Venlafaxine is currently marketed for treatment of depressive disorders as a conventional tablet formulation with a twice or three times daily dosage regimen. The absolute bioavailability of the conventional (CF) and extended-release (XR) formulations and their effects on electroencephalograms (EEG) and on a visual analog scale (VAS) for nausea were assessed in a randomized, double-blind, four-way crossover, placebo-controlled study of 16 healthy young men who were given either a single oral dose of 50 mg of CF venlafaxine, 75 mg of XR venlafaxine, or an intravenous dose of 10 mg of venlafaxine, or a placebo at 1-week intervals. The absolute bioavailability of venlafaxine was between 40% and 45% and was similar for both the CF and XR formulations. Venlafaxine produced central effects of a desipramine-like antidepressant. Regardless of formulation tested, the main EEG changes were an increase in fast beta (20-30 Hz) energy, which was more pronounced over the frontotemporal regions and extended within the full beta range (16-40 Hz). Maximum effect was reached at 6 hours for the CF and reached a plateau from 10 to 24 hours for the XR formulation. A dose-proportional increase in central activity, expressed as area under the effect curve (AUE) of the beta band, was observed between the CF (50 mg) and XR (75 mg) formulations. Compared with the CF tablet, the XR formulation also produced a much less intense maximum effect and a decrease of 63% in the AUE of nausea normalized by dose. The XR formulation has the same absolute bioavailability and the same central activity as assessed by EEG, but produced less intensive nausea than CF venlafaxine. The present findings suggest that a once-daily dosage regimen should be sufficient. This was confirmed by several clinical trials in depressive patients.

Published

1998

10. Population pharmacokinetics of intravenous amiodarone and comparison with two-stage pharmacokinetic analysis.

Author

Vadiei K, Troy S, Korth-Bradley J, Chiang ST, and Zimmerman JJ

Subjects

Adult, Aged, Aged, 80 and over, Amiodarone administration & dosage, Anti-Arrhythmia Agents administration & dosage, Female, Humans, Injections, Intravenous, Kidney Diseases metabolism, Male, Middle Aged, Ventricular Dysfunction, Left metabolism, Amiodarone pharmacokinetics, Anti-Arrhythmia Agents pharmacokinetics

Abstract

The disposition of amiodarone, an antiarrhythmic agent was evaluated after a single intravenous infusion (5 mg/kg over 15 minutes) in patients of various ages and with various degrees of renal function and left ventricular function. The plasma concentration-time data were obtained from three clinical studies with similar protocols. The data were analyzed by nonlinear mixed-effects modeling (NONMEM) to estimate the population pharmacokinetic parameters of amiodarone and to determine the significant demographic covariates affecting these parameters. The pharmacokinetic parameters of amiodarone (weight-corrected) also were calculated using two-stage analysis and were compared with the results obtained from the mixed-effects analysis. The population plasma concentration-time profile of amiodarone was best described by a four-compartment model. Demographic covariates (i.e., creatinine clearance and ejection fraction) did not improve the final pharmacostatistical model significantly. The results from the two-stage analysis showed no significant relationship between amiodarone pharmacokinetic parameters and age, gender, renal function, or ejection fraction. The results from one study, however, demonstrated that advanced age (> or = 65 years) resulted in reduced amiodarone clearance coupled with a prolonged elimination half-life. No such correlation was detected with NONMEM analysis, which may be partly attributable to the small number of elderly patients. Overall, the results from NONMEM analysis validated the results obtained from the two-stage analysis.

Published

1997

11. Pharmacokinetics of the aldose reductase inhibitor tolrestat: studies in healthy young and elderly male and female subjects and in subjects with diabetes.

Author

Fruncillo R, Troy S, Parker V, Mayersohn M, Hicks D, Kraml M, Battle M, and Chiang S

Subjects

Administration, Oral, Adult, Aged, Chromatography, High Pressure Liquid, Diabetes Mellitus metabolism, Enzyme Inhibitors blood, Enzyme Inhibitors therapeutic use, Female, Half-Life, Humans, Intestinal Absorption, Male, Metabolic Clearance Rate, Middle Aged, Naphthalenes blood, Naphthalenes therapeutic use, Sex Factors, Aging metabolism, Aldehyde Reductase antagonists & inhibitors, Diabetes Mellitus drug therapy, Enzyme Inhibitors pharmacokinetics, Naphthalenes pharmacokinetics

Abstract

Tolrestat is an aldose reductase inhibitor undergoing clinical trials in diabetic subjects that may reduce the severity of chronic tissue damage associated with hyperglycemia. These studies were conducted to evaluate the pharmacokinetics of tolrestat in healthy young and elderly male and female subjects and in young and elderly subjects with diabetes. The drug was administered in a multiple-dose regimen, and steady-state parameters were obtained. There were no important gender-related differences, but mean values for apparent oral clearance, renal clearance, and corresponding unbound parameters were significantly lower for the elderly healthy subjects than for the young healthy subjects. The drug is highly bound to plasma proteins, and the unbound fraction (0.75%) did not differ among the subjects. The results from young and elderly diabetic subjects suggest that diabetes per se has no influence on tolrestat disposition but that there is an age-related reduction in apparent oral clearance (30 versus 18 ml/hr/kg) and a corresponding increase in the minimum steady-state plasma concentration (1.2 versus 1.9 micrograms/ml). These data indicate a possible need to reduce the dose of tolrestat in elderly subjects, assuming the same concentration-response relationship.

Published

1996

12. The dose proportionality of the pharmacokinetics of ardeparin, a low molecular weight heparin, in healthy volunteers.

Author

Troy S, Fruncillo R, Ozawa T, Mammen E, Holloway S, and Chiang S

Subjects

Adult, Cross-Over Studies, Factor Xa Inhibitors, Heparin, Low-Molecular-Weight administration & dosage, Humans, Male, Prothrombin antagonists & inhibitors, Fibrinolytic Agents pharmacokinetics, Heparin, Low-Molecular-Weight pharmacokinetics

Abstract

Ardeparin is a low molecular weight heparin currently being evaluated as an antithrombotic agent. The objective of this investigation was to assess the effects of dose on the pharmacokinetics of ardeparin after subcutaneous administration. Eighteen healthy subjects received doses of 30 U/kg, 60 U/kg, and 100 U/kg antifactor Xa (aXa) of ardeparin by subcutaneous injection. Plasma antifactor IIa (aIIa) activity levels after the 30- and 60-U/kg doses of ardeparin were too low to reliably characterize the disposition of the drug. However, the pharmacokinetics of ardeparin could be characterized by using pharmacodynamic measurements of plasma aXa activity. The rate of absorption of ardeparin after subcutaneous administration did not change with increasing dose. The volume of distribution (Vd) of ardeparin was small, reflecting minimal distribution outside the intravascular space, and was independent of dose. The total clearance of ardeparin, however, decreased with increasing dose, and half-life (t1/2) was prolonged at the higher doses. Within the observed dose range, a doubling of the ardeparin dose resulted in an area under the plasma aXa activity-versus-time curve (AUC) that was approximately 25% greater than expected on the basis of linear disposition. The differences in AUC and clearance between the three doses suggest that the mechanism of elimination of ardeparin is saturable.

Published

1995