Conformationally restricted psychoactive agents

Paradkar, Vidyadhar Madhav

January 1979

No description available.

Neuropsychopharmacology.

Antidepressants.

Tranquilizing drugs.

Synthetic and spectroscopic studies of 1,4-benzodiazepine analogues

Mphahlele, Malose Jack

January 1994

In this project, an extensive range of benzodiazepine analogues have been synthesised via Schmidt reaction of specially prepared flavanone, 4-quinolone and l-thioflavanone precursors; nitrogen insertion being effected by use of trimethylsilyl azide in trifluoroacetic acid. In some cases, several of the benzodiazepine analogues have also been prepared by alternative cyclisation routes. A detailed kinetic-mechanistic study of the Schmidt reaction of flavanones has been carried out using 'H NMR spectroscopy to explain the observed regiochemistry of nitrogen insertion. The reaction rates, for the formation of both amide and tetrazolo derivatives have been found to be influenced by the electronic effects of the A- and B-ring substituents. A series of benzodiazepine analogues have been shown to undergo regioselective A-ring chlorination with t-butylhypochlorite; the products being characterised by 'H NMR, IR and mass spectroscopy. The mass spectrometric fragmentation patterns of series of 2-aryl-4-quinolones, and 2-aryl-l ,4-benzodiazepinones and their tetrazolo[l ,5-dl analogues have been elucidated using a combination of low-resolution, high-resolution and metastable-peak analyses. The binding affinities of various benzodiazepine analogues for rat brain benzodiazepine receptors have been evaluated using a radioreceptor assay technique. Structure-activity relationships were investigated to establish the effects of various A-, B- and Coring substituents on binding affinity. The conformational preferences of selected systems have been studied using a combination of multi-pulse 'H NMR spectroscopy, X-ray crystallography and computer modelling techniques with a view to establishing the influence of conformation on binding affinity.

Benzodiazepines

Tranquilizing drugs

A depressive effect of librium on problem-solving incentive/

Lewis, Everett Mercer

01 January 1963

No description available.

Learning

Psychology

Tranquilizing drugs

The effect of chlordiazepoxide on the stimulus-intensity phenomenon.

Green, Donald Ray

01 January 1964

No description available.

Behaviorism (Psychology

Tranquilizing drugs)

The effect of chlordiazepoxide on acquisition and extinction responding for rewarding brain stimulation.

Gandelman, Ronald.

01 January 1968

No description available.

Behaviorism (Psychology

Tranquilizing drugs)

Pharmacokinetic properties of meprobamate in the dog; an example of dose-dependency in elimination kinetics.

Martis, Leo.

January 1973

Thesis (Ph. D.)--University of Washington. / Bibliography: l. [116]-121.

Can a horse learn while under the influence of a tranquilizer (Acepromazine maleate)

Griffith, Samantha C., McCall, Cynthia Ann.

January 2006

Thesis(M.S.)--Auburn University, 2006. / Abstract. Vita. Includes bibliographic references.

Minor tranquilziers [sic] and the Valium epidemic prescription drug use and abuse in the United States, 1906-1979 /

Fruhwirth, Grant.

January 2010

Thesis (M.A. in history)--Washington State University, May 2010. / Title from PDF title page (viewed on July 6, 2010). "Department of History." Includes bibliographical references (p. 122-129).

THE EFFECTS OF A SHORT-ACTING BENZODIAZEPINE, TRIAZOLAM, ON AROUSALS, BODY MOVEMENTS, AND QUALITY OF SLEEP IN POSTMENOPAUSAL FEMALES.

DAVIS-SHARTS, JEAN ELIZABETH.

January 1987

The purpose of this study was to determine the effects of triazolam, a short-acting benzodiazepine, on nocturnal arousals, body movements, and quality of sleep in healthy, postmenopausal females. A double-blind control by constancy cross-over design was employed. Twelve subjects were randomly assigned to the sequence paradigm placebo, drug, placebo, drug or to the sequence paradigm drug, placebo, drug, placebo. Each subject slept for six nights in a sleep laboratory that was specifically designed to decrease the artificiality of the laboratory setting. EEG, EOG, and EMG measurements were recorded on a polysomnograph. Body movements were recorded on videotape and measured by radar and ultrasound instruments. Sleep quality was measured using both Likert and visual analogue scales. In examining arousal activity during sleep period time, the findings demonstrated a significant decrease in wakes after sleep onset (WASO), sleep stage one episodes, and sleep stage shifts when triazolam was compared to a placebo reference. There was no significant effect on K-complex activity associated with movement. In examining body movements during the sleep period time, the findings demonstrated a significant decrease in major body movements when triazolam was compared to a placebo reference. Minor body movements were increased, but not at significant levels. In examining the subject's perceived quality of sleep, their satisfaction with sleep was significantly increased on nights following triazolam administration when compared with nights following placebo administration.

Benzodiazepines.

Tranquilizing drugs.

Hypnotics.

Sleep -- Age factors.

Approaches to the synthesis of pentacyclic dibenzazepines and phenothiazines.

Dunbar, Philip Gordon.

January 1987

Rigid analogues of the tricyclic antidepressant imipramine and the phenothiazine tranquilizer promazine were designed and their syntheses were attempted. Conformational rigidity was expected to reduce the side effects of these drugs by limiting their binding to multiple receptors. Ortho-directed metalation followed by acylation provided synthetic intermediates for the formation of the desired pentacyclic congeners. The known dilithiation of phenothiazine and iminodibenzyl and n-butyllithium, followed by acylation with dimethylformamide, gave carboxaldehydes at the 1 and 4 positions respectively. Ortho-lithiated nicotinamides were acylated by these aldehydes exclusively at the 4 position to provide the key intermediate alcohol amides. Difficulties in amide hydrolysis are discussed. Catalytic hydrogenation over palladium-on-carbon in refluxing acetic acid yielded carboxylic acids, apparently via the gamma-lactones formed in situ. The lactones could not be isolated easily due to instability to oxidation. Pentacyclic lactams were formed by dehydration, and borane was used to reduce the carbonyl function. Only the iminodibenzyl lactam was reduced, and problems encountered in subsequent pyridine ring reduction are discussed. Cis and trans ring fusion isomers were identified by ¹³C nmr. Attempted one-pot synthesis of this pentacycle and a regioisomer by double acylation of 4,5-dilithioiminodibenzyl with 2,3-pyridinedicarboxylic anhydride, and 3,4-pyridinedicarboxylic anhydride failed. Mechanistic considerations are discussed regarding regiochemistry and reactivity of the nitrogen and carbon anions involved. Ortho-lithiation of 3-bromopyridine to form 3-pyridyne in the presence of the preformed N-lithioiminodibenzyl-4-carboxaldehyde was unsuccessful in providing a pentacyclic benzonaphthyridinobenzazepine. The resulting 2- and 4-lithiated 3-bromopyridines were trapped by the aldehyde instead. Both hydroxymethylbromopyridines were identified by their proton coupling patterns in the pyridine ring. These compounds are discussed as potential precursors to pentacyclic benzazepinopyridobenzazepines. Several other attempts at forming benzonaphthyridinobenzazepines and naphthyridinophenothiazines were unsuccessful. Intermediates were obtained by carbon acylation of the dilithiated iminodibenzyl and phenothiazine with arecoline esters, arecaidine, and pyridine-3-carboxaldehyde. Dibenzylic alcohol reduction is discussed, as is its labile oxidation. None of the resulting pyridylmethyl heterocycles could be cyclized.

Benzodiazepines.

Tranquilizing drugs.

Psychotropic drugs.

Antidepressants.