Abstract
In the elevated plus-maze test of anxiety the scores of control animals remain stable over repeated tests. However, a single prior exposure to the plus-maze renders an animal insensitive to the anxiolytic effects of chlordiazepoxide. This phenomenon of “one-trial tolerance” persisted even when the two trials were separated by as much as 2 weeks. It has previously been shown that the drug state of the animal on trial 1 is not important to the development of the phenomenon, but one-trial tolerance did not develop if a very high dose (75 mg/kg) of chlordiazepoxide was given on trial 1; it is suggested that this is due to the amnesic effects of the drug. The learning on trial 1 was not specific to a particular plus-maze and tolerance could be observed even when the maze on trial 1 was made from different material. The crucial experience on trial 1 was experience of an open arm of the maze. Whereas tolerance could be obtained as a result of a previous plus-maze experience, there was no evidence of an anxiogenic withdrawal response when rats were tested the following day undrugged. The phenomenon of one-trial tolerance is explained within our recently proposed two-factor theory of benzodiazepine dependence; it is suggested that one-trial tolerance provides a method for studying the mechanism underlying the development of tolerance to anxiolytic effects, independently from the mechanism underlying the development of withdrawal responses.
This is a preview of subscription content, log in via an institution to check access.
Similar content being viewed by others
References
Cooper SJ, Burnett G, Brown K (1981) Food preference following acute or chronic chlordiazepoxide administration: tolerance to an antineophobic action. Psychopharmacology 73:70–74
File SE (1985) Tolerance to the behavioral actions of benzodiazepines. Neurosci Biobehav Rev 9:113–121
File SE (1990) One-trial tolerance to the anxiolytic effects of chlordiazepoxide in the plus-maze. Psychopharmacology 100:281–282
File SE, Baldwin HA (1989) Changes in anxiety in rats tolerant to, and withdrawn from, benzodiazepines: behavioural and biochemical studies. In: Tyrer P (ed) Psychopharmacology of anxiety. Oxford University Press, Oxford, pp 28–51
File SE, Hitchcott PK (1990) A theory of benzodiazepine dependence that can explain whether flumazenil will enhance or reverse the phenomena. Psychopharmacology (in press)
File SE, Baldwin HA, Aranko K (1987) Anxiogenic effects from benzodiazepine withdrawal are linked to the development of tolerance. Brain Res Bull 19:607–610
Gallager DW, Lakoski JM, Gonsalves SF, Rauch SL (1984) Chronic benzodiazepine treatment decreases postsynaptic GABA sensitivity. Nature 308:74–77
Gonzales JP, McCulloch AJ, Nicholls PJ, Sewell RDE, Tekle A (1984) Subacute benzodiazepine treatment: observations on behavioural tolerance and withdrawal. Alcohol Alcohol 19:325–332
Lister RG (1985) The amnesic effects of benzodiazepines in man. Neurosci Biobehav Rev 9:87–94
Lister RG (1987) The use of a plus-maze to measure anxiety in the mouse. Psychopharmacology 92:180–185
Pellow S, Chopin P, File SE, Briley M (1985) Validation of open: closed arm entries in an elevated plus-maze as a measure of anxiety in the rat. J Neurosci Methods 14:149–167
Soderpalm B (1987) Pharmacology of the benzodiazepines, with special emphasis on alprazolam. Acta Psychiatr Scand 76:39–46
Treit D (1985) Evidence that tolerance develops to the anxiolytic effect of diazepam in rats. Pharmacol Biochem Behav 22:383–387
Vellucci SV, File SE (1979) Chlordiazepoxide loses its anxiolytic action with long-term treatment. Psychopharmacology 62:61–65
Author information
Authors and Affiliations
Rights and permissions
About this article
Cite this article
File, S.E., Mabbutt, P.S. & Hitchcott, P.K. Characterisation of the phenomenon of “one-trial tolerance” to the anxiolytic effect of chlordiazepoxide in the elevated plus-maze. Psychopharmacology 102, 98–101 (1990). https://doi.org/10.1007/BF02245751
Received:
Revised:
Issue Date:
DOI: https://doi.org/10.1007/BF02245751