Martha Sanchez-Craig
University of Toronto
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Featured researches published by Martha Sanchez-Craig.
The New England Journal of Medicine | 1986
Usoa E. Busto; Edward M. Sellers; Claudio A. Naranjo; Howard Cappell; Martha Sanchez-Craig; Kathy Sykora
We conducted a double-blind, placebo-controlled trail in which 40 patients who had undergone long-term therapy with benzodiazepines were switched to placebo or to diazepam in a dose approximately equivalent to their usual dose of the benzodiazepine; the dose of diazepam was then tapered during an eight-week period. Patients were assessed clinically and psychologically and had weekly sessions of behavioral therapy. The subjects who received placebo had more symptoms, assessed their symptoms as more severe, and stopped taking the study drug at a higher rate than those receiving the tapering doses of diazepam. The subjects in the placebo group also had symptoms shortly after being switched to placebo, whereas those in the diazepam group had symptoms much later. Some withdrawal symptoms were distinct from those of anxiety (e.g., tinnitus, involuntary movement, and perceptual changes). Withdrawal symptoms occurred earlier in patients who had received short-acting benzodiazepines than in those who had received long-acting benzodiazepines. Symptoms gradually disappeared over a four-week period in both the placebo and the diazepam groups. Serial determination of plasma benzodiazepine concentrations was a useful way to assess compliance, treatment outcome, and relapse during withdrawal. We conclude that a clinically important, mild, but distinct withdrawal syndrome occurs after discontinuation of long-term therapeutic use of benzodiazepines.
Clinical Pharmacology & Therapeutics | 1984
Claudio A. Naranjo; Edward M. Sellers; Carol Roach; Denise V Woodley; Martha Sanchez-Craig; Kathy Sykora
The effect of zimelidine, a specific serotonin‐reuptake inhibitor, on alcohol intake was tested in 13 healthy male, nondepressed heavy drinkers who were randomly allocated to receive zimelidine or placebo in a double‐blind, crossover experiment. There were five 2‐wk experimental periods (baseline, placebo 1 and 2, and zimelidine 1 and 2). Treatment was discontinued in three subjects due to a suspected adverse reaction and three other subjects dropped out. Thus, 13 subjects participated in at least two experimental drug periods and only 10 participated in all the periods. In the 13 subjects zimelidine increased the days of abstinence and decreased the daily number of drinks consumed, whereas in the 10 subjects only the number of days of abstinence increased. Subjects did not report aversive alcohol‐sensitizing reactions. Spielberger state‐anxiety test scores and depression scores (Montgomery/Asberg and Hamilton) were low at the beginning and throughout the study. Our data suggest that zimelidine modifies alcohol intake by a different mechanism than previously tested drugs, possibly by modulating the central neural mechanism that controls drinking of alcohol.
Addiction | 1989
Martha Sanchez-Craig; Gillian M. Leigh; Karen Spivak; Hau Lei
Addiction | 1986
Usoa E. Busto; Edward M. Sellers; Claudio A. Naranjo; Howard Cappell; Martha Sanchez-Craig; Jan Simpkins
Addiction | 1991
Martha Sanchez-Craig; Karen Spivak; Rafaela Davila
Addiction | 1986
Martha Sanchez-Craig; Hau Lei
Journal of Consulting and Clinical Psychology | 1996
Martha Sanchez-Craig; Rafaela Davila; Gerald Cooper
Addiction | 1990
Martha Sanchez-Craig
Addiction | 1986
Martha Sanchez-Craig
Psychopharmacology | 1987
Howard Cappell; Usoa E. Busto; Gloria Kay; Claudio A. Naranjo; Edward M. Sellers; Martha Sanchez-Craig