1992
DOI: 10.1016/0006-8993(92)90914-u
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Citalopram's ability to increase the extracellular concentrations of serotonin in the dorsal raphe prevents the drug's effect in the frontal cortex

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Cited by 265 publications
(186 citation statements)
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“…Pretreatment with 1-10 mg/kg citalopram, i.e., doses that increase extracellular 5-HT levels in different brain regions with maximal effects, 1 h after systemic administration (for example, Invernizzi et al 1992;Hjorth 1993), increased in a dose-dependent manner midbrain 5-HT levels in all strains, either to significant (SHRs and WKY rats) or to non significant (LEW rats) extents. In addition, the reductions in 5-HIAA levels were already maximal with the lowest dose of citalopram in SHRs (as revealed by the lack of statistical difference between citalopram-treated groups), an observation that could be extended to hippocampal 5-HIAA levels.…”
Section: Strain-related Differences In the Effects Of Citalopram On Cmentioning
confidence: 99%
“…Pretreatment with 1-10 mg/kg citalopram, i.e., doses that increase extracellular 5-HT levels in different brain regions with maximal effects, 1 h after systemic administration (for example, Invernizzi et al 1992;Hjorth 1993), increased in a dose-dependent manner midbrain 5-HT levels in all strains, either to significant (SHRs and WKY rats) or to non significant (LEW rats) extents. In addition, the reductions in 5-HIAA levels were already maximal with the lowest dose of citalopram in SHRs (as revealed by the lack of statistical difference between citalopram-treated groups), an observation that could be extended to hippocampal 5-HIAA levels.…”
Section: Strain-related Differences In the Effects Of Citalopram On Cmentioning
confidence: 99%
“…The 5-HT elevations in frontal cortex and raphe nuclei were comparable. This regional selectivity is different from that of agents that selectively block 5-HT reuptake, which enhances extracellular 5-HT more in the raphe nuclei than in frontal cortex (Adell and Artigas 1991; Bel and Artigas 1992;Invernizzi et al 1992;Malagié et al 1995;Hervás and Artigas 1998).…”
Section: Discussionmentioning
confidence: 86%
“…The 5-HT elevations in frontal cortex and raphe nuclei were comparable. This regional selectivity is different from that of agents that selectively block 5-HT reuptake, which enhances extracellular 5-HT more in the raphe nuclei than in frontal cortex (Adell and Artigas 1991; Bel and Artigas 1992;Invernizzi et al 1992;Malagié et al 1995;Hervás and Artigas 1998).Milnacipran markedly elevated the 5-HT output in rat brain when administered by reverse dialysis (7-and 10-fold in frontal cortex and midbrain, respectively). The antagonism of this effect by the omission of Ca 2ϩ ions and the addition of TTX indicates that milnacipran elevated the 5-HT output by blockade of the reuptake of the 5-HT released by an impulse-dependent mechanism and not by a fenfluramine-like releasing action, because the latter is insensitive to the blockade of nerve transmission (Carboni and Di Chiara 1989).…”
mentioning
confidence: 81%
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“…Neurochemical studies have shown that antidepressant drugs that inhibit the serotonin transporter (e.g., SSRIs and certain tricyclics) preferentially increase the concentration of extracellular serotonin in the midbrain raphe, presumably because this region has the highest density of serotonin uptake sites in the brain (Adell and Artigas 1991;Invernizzi et al 1992;Artigas 1993;Hervás and Artigas 1998). The increase in raphe serotonin leads to an inhibition of serotonergic neuronal activity through enhanced activation of somatodendritic 5-HT 1A autoreceptors (Blier and de Montigny 1994).…”
Section: Discussionmentioning
confidence: 99%