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Titlebook: Anxiolytic β-Carbolines; From Molecular Biolo David N. Stephens Book 1993 Springer-Verlag Berlin Heidelberg 1993 Beta Carboline.GABA.anxiet

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Messung der Induktionskoeffizienten,hermore, again unlike full agonists, physical dependence could not be induced in squirrel monkeys after repeated very high doses of bretazenil as assessed by challenge with the BZ-receptor antagonist, flumazenil (Haefely et al. 1990). Although these data on bretazenil indicate that partial BZ-recept
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https://doi.org/10.1007/978-3-642-48064-5and the reinstatement of the drug of dependence terminates the symptoms. Thus, we have argued that the occurrence of anxiety, a key symptom of benzodiazepine withdrawal, may be critical in the maintenance of chronic benzodiazepine taking (Emmett-Oglesby et al. 1990).
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Molecular Biology of Gamma-Aminobutyric Acid Type A/Benzodiazepine Receptors, years, mainly as a result of modern molecular-biology techniques, the understanding of the pharmacology, biochemistry, and electrophysiology of these channels has advanced greatly. The family of ligand-gated ion channels now comprises the molecularly related nicotinic acetylcholine receptors (AChR)
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Abecarnil is a Full Agonist at Some, and a Partial Agonist at Other Recombinant GABAA Receptor Subtine-gated ion channels reduces neuronal excitability. These anion channels belong to a ligand-gated ion channel family and are formed by pentamers of five membrane-spanning subunits. For the vertebrate GABA. receptor, 16 such receptor subunits, divided by sequence and functional homology into five c
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Abecarnil: A Novel Anxiolytic with Mixed Full Agonist/Partial Agonist Properties in Animal Models omber of properties which limit their use or which give rise to problems on withdrawal. Thus, currently available benzodiazepine anxiolytics are sedative and muscle relaxant, induce memory impairment, increase the intoxicating potency of alcohol, may be subject to nontherapeutic use (abuse), and, fol
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Abecarnil Shows Reduced Tolerance Development and Dependence Potential in Comparison to Diazepam: Arer 1983; Woods et al. 1987; Haefely et al. 1990). Recent reports have indicated that partial (low efficacy) BZ-receptor agonists, i. e., compounds which induce smaller fractional responses in their target cells than do full agonists at the same fractional receptor occupancy, may have advantages in
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