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Your search keyword '"Snavely, Duane B."' showing total 24 results
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24 results on '"Snavely, Duane B."'

1. Suvorexant in Patients with Insomnia: Pooled Analyses of Three-Month Data from Phase-3 Randomized Controlled Clinical Trials.

Author

Herring, W Joseph, Connor, Kathleen M, Snyder, Ellen, Snavely, Duane B, Zhang, Ying, Hutzelmann, Jill, Matzura-Wolfe, Deborah, Benca, Ruth M, Krystal, Andrew D, Walsh, James K, Lines, Christopher, Roth, Thomas, and Michelson, David

Subjects
Humans, Sleep Initiation and Maintenance Disorders, Azepines, Triazoles, Treatment Outcome, Double-Blind Method, Dose-Response Relationship, Drug, Adolescent, Adult, Aged, Middle Aged, Female, Male, Young Adult, Sleep Aids, Pharmaceutical, insomnia, orexin, pharmacotherapy, randomized controlled trial, sleep, suvorexant, Aging, Clinical Trials and Supportive Activities, Neurosciences, Sleep Research, Clinical Research, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Clinical Sciences, Other Medical and Health Sciences, Psychology, Neurology & Neurosurgery
Abstract

Study objectivesSuvorexant is an orexin receptor antagonist approved for treating insomnia at a maximum dose of 20 mg. Phase-3 trials evaluated two age-adjusted (non-elderly/elderly) dose-regimes of 40/30 mg and 20/15 mg with the primary focus on 40/30 mg. We report here results from pooled analyses of the 20/15 mg dose-regime, which was evaluated as a secondary objective in the trials.MethodsPrespecified analysis of pooled data from two identical randomized, double-blind, placebo-controlled, parallel-group, 3-month trials in non-elderly (18-64 years) and elderly (≥ 65 years) patients with insomnia. Patients were randomized to suvorexant 20/15 mg (non-elderly/elderly), suvorexant 40/30 mg (non-elderly/elderly), or placebo; by design, fewer patients were randomized to 20/15 mg. Efficacy was assessed by self-reported and polysomnography (PSG; subset of patients) sleep maintenance and onset endpoints.ResultsSuvorexant 20/15 mg (N = 493 treated) was effective compared to placebo (N = 767 treated) on patient-reported and PSG sleep maintenance and onset endpoints at Night-1 (PSG endpoints) / Week-1 (subjective endpoints), Month-1 and Month-3, except for effects on PSG sleep onset at Month-3. Suvorexant 20/15 mg was generally well tolerated, with 3% of patients discontinuing due to adverse events over 3 months vs. 5.2% on placebo. Somnolence was the most common adverse event (6.7% vs. 3.3% for placebo). There was no systematic evidence of rebound or withdrawal signs or symptoms when suvorexant was discontinued after 3 months of nightly use.ConclusionsSuvorexant 20/15 mg improved sleep onset and maintenance over 3 months of nightly treatment and was generally safe and well tolerated.Clinical trial registrationClinicalTrials.gov trial registration numbers: NCT01097616, NCT01097629.

Published
2016

11. Suvorexant in Patients With Insomnia: Results From Two 3-Month Randomized Controlled Clinical Trials

Author

Herring, W. Joseph, primary, Connor, Kathryn M., additional, Ivgy-May, Neely, additional, Snyder, Ellen, additional, Liu, Ken, additional, Snavely, Duane B., additional, Krystal, Andrew D., additional, Walsh, James K., additional, Benca, Ruth M., additional, Rosenberg, Russell, additional, Sangal, R. Bart, additional, Budd, Kerry, additional, Hutzelmann, Jill, additional, Leibensperger, Heather, additional, Froman, Samar, additional, Lines, Christopher, additional, Roth, Thomas, additional, and Michelson, David, additional

Published
2016
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16. Addition of an NK1 receptor antagonist to an SSRI did not enhance the antidepressant effects of SSRI monotherapy: results from a randomized clinical trial in patients with major depressive disorder.

Author

Ball, William A., Snavely, Duane B., Hargreaves, Richard J., Szegedi, Armin, Lines, Christopher, and Reines, Scott A.

Subjects
*SUBSTANCE P receptors, *SEROTONIN uptake inhibitors, *RANDOMIZED controlled trials, *PAROXETINE, *DEPRESSED persons
Abstract

Objective Aprepitant is a neurokinin 1 receptor antagonist approved for prevention of chemotherapy-induced and post-operative nausea and vomiting. Early studies demonstrated promising antidepressant activity as monotherapy, although this was unsupported by subsequent phase 3 trials. This phase 2 study evaluated whether aprepitant potentiated the antidepressant effects of paroxetine. Methods Outpatients with major depressive disorder were randomized to aprepitant 200 mg + paroxetine 20 mg, paroxetine + placebo, or aprepitant + placebo for 6 weeks. The primary endpoint was change in HAMD-17 total score. Secondary/exploratory endpoints included changes in HAMA, CGI-S, CGI-I, and HAMD Item-1 scores at week 6. Results A total of 79, 78, and 79 patients received aprepitant + paroxetine, paroxetine + placebo, and aprepitant + placebo, respectively. At week 6, mean changes in HAMD-17 were −11.0 (95% confidence interval [CI]: −12.7, −9.4), −11.7 (95% CI: −13.3, −10.0), and −9.5 (95% CI: −10.9, −8.1), respectively. Pairwise comparisons of HAMD-17 change with combination therapy versus paroxetine alone demonstrated no significant difference ( p = 0.567). Changes in CGI-S, CGI-I, and HAMD Item-1 scores were also comparable, although there was a greater reduction in anxiety (HAMA) with paroxetine alone than aprepitant + paroxetine ( p = 0.045). Adverse events were generally more common with the combination than either monotherapy. Conclusion Concomitant use of aprepitant + paroxetine for 6 weeks did not provide greater antidepressant benefit compared with paroxetine + placebo in patients with major depression. Copyright © 2014 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published
2014
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19. A Statistics Appreciation Course for Clinical Research Personnel

Author

Bradstreet, Thomas E., primary, Belliel, Susan Linna, additional, Berman, Rayanne S., additional, Copenhaver, Margaret DiPonzio, additional, Hesney, Michael, additional, Holder, Daniel, additional, Hufnagel, Karen E., additional, Kersh, Louisa L., additional, Liss, Charles L., additional, Neafus, Richard P., additional, Payne, J. Ellen, additional, Schwartz, Skai W., additional, Snavely, Duane B., additional, Suchower, Lisa J., additional, and Walton-Bowen, Karen L., additional

Published
1992
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23. Development and persistence of antibody in a high risk institutionalized population given plasma-derived hepatitis B vaccine

Author

West, David J., Snavely, Duane B., Zajac, Barbara A., Brown, George W., and Babb, C.Jean

Abstract

Three hundred and twenty-two (322) persons with severe mental handicaps were given plasma-derived hepatitis B vaccine (20 μg dose at 0, 1 and 6 months). Following the third injection, 95% of the vaccinees were positive for anti-HBs, while 92% achieved a protective level of antibody (⩾ 10 mIU ml−1) with a geometric mean titre of 2568 mlU ml−1. Females responded better than males. Antibody responses declined with increasing age in both sexes, but they were not significantly influenced by body weight. Persistence of antibody in responders was followed over 4 years. The proportion of responders maintaining ⩾ 10 mIU ml−1was a function of initial antibody titre but was not significantly affected by sex, age or body weight. Overall, 76% of the responders are estimated to have ⩾ 10 mIU ml−1of anti-HBs 4 years after the first injection of vaccine.

Published
1990
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