Norfluoxetine Enantiomers as Inhibitors of Serotonin Uptake in Rat Brain

Wong, David T.; Bymaster, Frank P.; Reid, Leroy R.; Mayle, Douglas A.; Krushinski, Joseph H.; Robertson, David W.

doi:10.1038/npp.1993.33

Cited by 104 publications

(62 citation statements)

References 13 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…R-FLX and S-FLX have similar affinity for the human 5-HT transporter and low affinity for the DA and NE transporters. Similar affinity of the enantiomers for 5-HT uptake has been found in studies utilizing monoamine uptake in rat synaptosomes (Wong et al 1993). However, stereoselectivity for human 5-HT 2A and 5-HT 2C receptors was found for R-FLX versus S-FLX with R-FLX having at least 20-fold higher affinity for the two receptors than S-FLX.…”

Section: Discussionsupporting

confidence: 74%

See 1 more Smart Citation

R-fluoxetine Increases Extracellular DA, NE, As Well As 5-HT in Rat Prefrontal Cortex and Hypothalamus An in vivo Microdialysis and Receptor Binding Study

Koch

2002

Neuropsychopharmacology

145

View full text Add to dashboard Cite

show abstract

Section: Discussionsupporting

confidence: 74%

“…The binding to rat 5-HT 3 receptors was from the method of Wong et al 1993. Inhibition of binding to 5-HT 4 and other neuronal receptors was provided by NovaScreen (Hanover, MD).…”

Section: Determination Of Binding To Neuronal Receptorsmentioning

confidence: 99%

R-fluoxetine Increases Extracellular DA, NE, As Well As 5-HT in Rat Prefrontal Cortex and Hypothalamus An in vivo Microdialysis and Receptor Binding Study

Koch

2002

Neuropsychopharmacology

145

View full text Add to dashboard Cite

show abstract

“…FLX and NFLX are known to be potent SSRIs (11). Thus, it was important to establish whether the difference between the S-and R-stereoisomers in eliciting a normalization of PTB action in SI mice was related to differences in 5-HT reuptake inhibition potency.…”

Section: Resultsmentioning

confidence: 99%

Fluoxetine and norfluoxetine stereospecifically facilitate pentobarbital sedation by increasing neurosteroids

Pinna

Costa

Guidotti

2004

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Mice housed in social isolation exhibit a decreased response to ␥-aminobutyric acid-mimetic drugs [i.e., pentobarbital (PTB)] associated with a down-regulation of telencephalic allopregnanolone (Allo) levels. In these mice, the PTB-induced loss of righting reflex is greatly reduced. Fluoxetine (FLX) and norfluoxetine (NFLX) stereospecifically reverse the effect of social isolation on the PTB-induced loss of righting reflex and on the decrease of telencephalic Allo content. The S-isomers of FLX and NFLX are 2-and 7-fold more potent, respectively, than their respective R-isomers. The EC 50s of FLX and NFLX required to normalize brain Allo content and PTB action are 10 -50 times lower than the IC 50s required for selective serotonin reuptake inhibitor activity. We conclude that normalization of PTB action elicited by the S-isomers of FLX and NFLX is related to the reversal of the down-regulation of brain Allo content and is independent of selective serotonin reuptake inhibitor activity. M ale mice that have been housed in social isolation (SI) for 15-30 days develop increased anxiety-related behaviors, respond aggressively to an intruder of the same sex (1-3), and display decreased responsiveness to drugs that stimulate ␥-aminobutyric acid type A (GABA A ) receptors, as shown by the shorter duration of the loss of righting reflex (RRL) induced by pentobarbital (PTB) or muscimol (1, 4).Several independent lines of evidence suggest that these effects are maintained in part by SI-induced down-regulation of neurosteroid biosynthesis. First, protracted SI decreases the telencephalic levels of allopregnanolone (Allo) (5), a neurosteroid that positively modulates the action of GABA and other GABA receptor ligands (i.e., muscimol or barbiturates) on GABA A receptors (6-9). Thus, reduced levels of Allo could mediate the SI-induced decrease in GABA responsiveness.Second, administration of SKF 105,111, a potent type I 5␣-reductase inhibitor, to naïve mice depletes brain Allo content by 60-80% in Ϸ1 h and concurrently reduces the duration of PTB-or muscimol-induced RRL (1, 4). In SI or SKF 105,111-treated mice, administration of Allo in doses that per se fail to change gross behavior normalizes the reduced action of muscimol or PTB (1, 4).Third, electrophysiological studies using the patch-clamp technique to record GABA-evoked Cl Ϫ currents from neocortical pyramidal neurons obtained from brain slices of mice in which the concentration of endogenous brain Allo was decreased by Ϸ80% after the administration of SKF 105,111 showed a reduction in the potency of exogenously applied GABA or muscimol to evoke Cl Ϫ currents (10). Furthermore, direct application of Allo to these slices reverted the dose-response curve of GABA toward the control profile of non-SKF 105,111-treated slices (10).Fourth, the administration of fluoxetine (FLX) to SI mice in doses that normalize brain Allo content reverses the reduced duration of PTB-induced RRL (1). The effect of FLX on brain Allo content is stereospecific; the S-isomers of FLX (S-FLX) and no...

show abstract

“…20) NDemethylation signiˆcantly contributes to produce active metabolites in cases of ‰uoxetine ( Fig. 1 (d)), 22,23) sibutramine, 24) ferroquine 25) and azonaˆde. 26) S-Oxidation of thioridazine and epoxidation of carbamazepine lead to the formation of mesoridazine 27) and carbamazepine-10, 11-epoxide, 28) respectively.…”

Section: Formation Of Pharmacologically Ac-tive Metabolitesmentioning

confidence: 99%

“…For instance, 3-hydroxyquinidine, 37) hydroxymetronidazole, 38) (R)-nor‰uoxetine, 22,23) norverapamil, 39) hydroxycyclosporine, 14) N-desmethylazonaˆde, 26) hydroxybupropion and threohydrobupropion, 18) and many active metabolites have weaker activities than their parents. But, in some cases, metabolites are more potent or have similar biological activities to parent drugs.…”

Section: Pharmacologically Active Metabo-lites Of Marketed Drugsmentioning

confidence: 99%

Pharmacologically Active Metabolites of Currently Marketed Drugs: Potential Resources for New Drug Discovery and Development

et al. 2010

View full text Add to dashboard Cite

Biotransformation is the major clearance mechanism of therapeutic agents from the body. Biotransformation is known not only to facilitate the elimination of drugs by changing the molecular structure to more hydrophilic, but also lead to pharmacological inactivation of therapeutic compounds. However, in some cases, the biotransformation of drugs can lead to the generation of pharmacologically active metabolites, responsible for the pharmacological actions. This review provides an update of the kinds of pharmacologically active metabolites and some of their individual pharmacological and pharmacokinetic aspects, and describes their importance as resources for drug discovery and development.

show abstract

Norfluoxetine Enantiomers as Inhibitors of Serotonin Uptake in Rat Brain

Cited by 104 publications

References 13 publications

R-fluoxetine Increases Extracellular DA, NE, As Well As 5-HT in Rat Prefrontal Cortex and Hypothalamus An in vivo Microdialysis and Receptor Binding Study

R-fluoxetine Increases Extracellular DA, NE, As Well As 5-HT in Rat Prefrontal Cortex and Hypothalamus An in vivo Microdialysis and Receptor Binding Study

Fluoxetine and norfluoxetine stereospecifically facilitate pentobarbital sedation by increasing neurosteroids

Pharmacologically Active Metabolites of Currently Marketed Drugs: Potential Resources for New Drug Discovery and Development

Contact Info

Product

Resources

About