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Dive into the research topics where Lori Merlotti is active.

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Featured researches published by Lori Merlotti.


Psychopharmacology | 1994

Sedative, memory, and performance effects of hypnotics

Timothy Roehrs; Lori Merlotti; Frank Zorick; Thomas Roth

The sedative, amnestic, and performance disruptive effects of benzodiazepine (Bz) receptor selective and non-selective hypnotics were studied in 23 healthy, normal subjects, aged 26.8±1.0 years. Triazolam (0.25 and 0.50 mg), zolpidem (10 and 20 mg) and placebo were administered, double-blind, at bedtime in a repeated measures design. During an awakening 90 min later (at approximate peak concentration of each drug) a 30-min performance battery which included memory, vigilance, and psychomotor tasks was completed. Each drug and dose impaired memory (both immediate and delayed), vigilance, and psychomotor performance relative to placebo. Among active drugs impairment was greatest with zolpidem 20 mg, next triazolam 0.50 mg, then zolpidem 10 mg, and finally triazolam 0.25 mg. Next morning delayed recall was also impaired by all drugs and doses (i.e. anterograde amnesia). The amnestic and performance-disruptive effects paralleled the relative hypnotic effects of the drugs and doses. No receptor selectivity in these pharmacodynamic effects was observed.


Journal of Clinical Psychopharmacology | 1989

The dose effects of zolpidem on the sleep of healthy normals.

Lori Merlotti; Timothy Roehrs; Gail Koshorek; Frank Zorick; James Lamphere; Thomas Roth

This study determined the dose effects of zolpidem in 12 healthy males with normal sleep patterns. Subjects spent 7 weeks, 3 consecutive nights per week, in the laboratory and had a 4-night washout between treatments. The first week was a screening and adaptation week. Then subjects received zolpidem (2.5, 5.0, 7.5, 10.0, or 20.0 mg) or placebo on the first two nights for each of the next 6 consecutive weeks. Treatments were organized in a Latin square design and administered in a double-blind fashion. On the third night of each treatment, subjects always received placebo. The 5.0 mg and larger doses of zolpidem significantly decreased latency to persistent sleep and wake before sleep. Sleep maintenance measures were not affected by zolpidem. The 7.5 mg and higher doses of zolpidem significantly increased total sleep time. The only significant sleep stage effect was a decrease in percent of rapid eye movement sleep at only the 20 mg dose. No consistent discontinuation effects were found. Zolpidem was hypnotically active at doses as low as 5.0 and 7.5 mg, and sleep stage effects occurred only at the 20 mg dose, thus separating the dose range of hypnotic and sleep stage effects.


Psychopharmacology | 1992

Rebound insomnia and hypnotic self administration

Timothy Roehrs; Lori Merlotti; Frank Zorick; Thomas Roth

Twenty-one (three groups of seven), men and women, 25–50 years of age were studied to determine whether or not rebound insomnia would increase the likelihood of self administering a benzodiazepine (triazolam 0.25 mg) hypnotic. The groups compared were patients with insomnia and disturbed sleep, insomnia and normal sleep, and healthy normals. Rebound insomnia, by both subjective and polysomnographic assessment, was induced. The experience of rebound insomnia did not increase the likelihood of self administering a benzodiazepine hypnotic in any of the groups. There were clear group differences in pill self administration with normals rarely and insomnia patients frequently, but not differentially (placebo versus active drug) self administering pills.


General Hospital Psychiatry | 1990

Subjective and Polysomnographic Characteristics of Patients Diagnosed with Narcolepsy

Leon Rosenthal; Lori Merlotti; David Young; Frank Zorick; Robert Wittig; Timothy Roehrs; Thomas Roth

In order to better characterize the subjective and polysomnographic findings in patients with narcolepsy, a follow-up questionnaire was mailed to all patients diagnosed with the disorder at the Henry Ford Hospital Sleep Disorders and Research Center. The questionnaire inquired regarding the present, previous, and change in status for the constellation of narcolepsy symptoms. Memory problems, problems of daytime function, and nocturnal sleep disturbance were included among the questions related to the symptomatic constellation. By definition, all patients were symptomatic of daytime sleepiness and were diagnosed with narcolepsy only if there were two or more rapid eye movement (REM) onsets documented on the polysomnographic evaluation. A high percentage of patients reported nocturnal sleep disturbance, which was one of the symptoms with the latest reported onset. Retrospective comparison of questionnaire responses to the clinical polysomnography revealed significantly more sleep maintenance difficulties in the group of patients reporting this symptom on the questionnaire. Patients with disturbed nocturnal sleep reported taking more naps during the day, although the Multiple Sleep Latency Test (MSLT) failed to show differences in sleep latency. Interestingly, this group of patients was found to have a significantly higher number of sleep onset REM episodes on the MSLT. Finally, the findings are discussed as they compare to studies that required the presence of cataplexy as part of their inclusion criteria.


Biological Psychiatry | 1990

Signs and symptoms associated with cataplexy in narcolepsy patients

Leon Rosenthal; Frank Zorick; Lori Merlotti; Robert Wittig; Timothy Roehrs; Thomas Roth

The purpose of this report is to compare the similarities and differences among patients with EDS, cataplexy, and polysomnographic evidence of narcolepsy with those without cataplexy but with all the other findings


Psychopharmacology | 1992

Rebound insomnia in normals and patients with insomnia after abrupt and tapered discontinuation

Timothy Roehrs; Lori Merlotti; Frank Zorick; Thomas Roth

Rebound insomnia was studied in subjects, aged 25–50 years, with insomnia complaints and normal sleep, insomnia complaints and disturbed sleep, and normal sleep with no complaints (N=21,n=7 per group). Standard sleep recordings were collected on a baseline night and after abrupt discontinuation of 6 nights of 0.50 mg triazolam, tapered discontinuation (3 nights of 0.50 mg, 2 nights of 0.25 mg, and 1 night of 0.125 mg triazolam) and 6 nights of placebo. Significantly disturbed sleep on the discontinuation night compared to the baseline night was found. The relative degree of rebound insomnia was greater in the abrupt condition than in either the tapered or placebo conditions. The tapered condition reduced sleep time by half that of the abrupt condition which was twice the reduction found in the placebo condition. An overall (regardless of group or condition) difference in baseline versus discontinuation sleep was found, suggesting that pill discontinuation itself leads to sleep disturbance. Subjects did not differ in rebound insomnia as a function of pre-existing sleep disturbance.


Sleep | 1994

Experimental sleep fragmentation.

Timothy Roehrs; Lori Merlotti; Nancie Petrucelli; Edward J. Stepanski; Thomas Roth


American Journal of Psychiatry | 1992

Long-term study of the sleep of insomnia patients with sleep state misperception and other insomnia patients

Rafael J. Salin-Pascual; Timothy Roehrs; Lori Merlotti; Frank Zorick; Thomas Roth


Chest | 1995

Effects of Theophylline on Nocturnal Sleep and Daytime Sleepiness/Alertness

Timothy Roehrs; Lori Merlotti; Donald Halpin; Leon Rosenthal; Thomas Roth


Sleep | 1996

Phase advance in moderately sleepy and alert normals

Timothy Roehrs; Raphael Salin-Pascual; Lori Merlotti; Leon Rosenthal; Thomas Roth

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Edward J. Stepanski

Rush University Medical Center

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