Befloxatone, a new reversible and selective
monoamine oxidase-A inhibitor
I. Biochemical profile
by
Curet O, Damoiseau G, Aubin N, Sontag N, Rovei V, Jarreau FX
Central Nervous System Research Department,
Synthelabo Recherche,
Rueil-Malmaison, France.
J Pharmacol Exp Ther 1996 Apr; 277(1):253-64
ABSTRACT
Befloxatone, a novel oxazolidinone derivative, inhibited selectively and
competitively monoamine oxidase (MAO)-A in human and rat brain, heart, liver and
duodenum homogenates with Ki values ranging from 1.9 to 3.6 nM for MAO-A and
from 270 to 900 nM for MAO-B. In vitro, befloxatone was more potent at
inhibiting MAO-A activity than reference compounds (befloxatone > harmaline
> brofaromine > BW 137OU87 > RS 8359 > toloxatone > moclobemide).
The inhibition of MAO-A by befloxatone was time-dependent and fully reversible
after dilution. After p.o. administration, befloxatone induced a dose-dependent
and selective inhibition of rat brain and duodenum MAO-A activities ex vivo with
ED50 values of 0.06 and 0.025 mg/kg, respectively. Befloxatone (0.5 mg/kg p.o.)
decreased MAO-B activity by only 20% in both tissues. In the brain, liver and
duodenum, the inhibition of MAO-A activity by befloxatone was short lasting.
Twenty-four hours after administration of befloxatone (0.75 mg/kg p.o.), a full
recovery of MAO-A activity was observed in the brain, but the enzyme activity
was still decreased by 38 and 56% in the duodenum and liver, respectively. In
the rat brain, befloxatone (0.75 mg/kg p.o.) increased levels of norepinephrine,
dopamine and 5-hydroxytryptamine and decreased levels of their respective
deaminated metabolites. These variations were dose-dependent and reversed 24 hr
after administration. In addition, befloxatone (0.75 mg/kg p.o.) decreased free
3,4-dihydroxyphenylethylene glycol levels in the brain and plasma. Befloxatone
(10 microM) did not modify the activities of diamine or benzylamine oxidase and
did not interact with monoamine uptake mechanisms or with a variety of
neurotransmitter or drug receptor sites. In conclusion, the neurochemical
profile of befloxatone demonstrates that this compound is a selective,
competitive, potent and reversible MAO-A inhibitor.
MAO
RIMAs
MAOIs
FA-70
Serotonin
Dopamine
Safinamide
Moclobemide
Norepinephrine
Moclobemide v tranylcypromine
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