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Discovery of Multi-functional Lead Compounds Originating from Traditional Chinese Medicine for Developing Anti-depressive Agents via Virtual Screening
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Background:
The increasing prevalence of depression has become a global health issue. Currently
approved anti-depressive including 5-hydroxytryptamine (5-HT), dopamine (DA), norepinephrine
(NE), triple reuptake inhibitors (TRIs) and glutamate N-methyl-D-aspartate (NMDA) receptor antagonists
have limited effects because of their insufficient efficacy and/or slow onset of action. Developing multifunctional
antidepressants that can modulate 5-HT, DA, NE, and NMDA simultaneously can potentially
overcome the current drug defects.
Objective:
This study aimed to explore leads for the development of multi-functional anti-depressive
agents that simultaneous triple reuptake inhibitory and NMDA-GluN2B receptor antagonistic activities.
Methods:
Potential leads were screened virtually from the TCMSP database based on the 3DPharmacophore
model of TRIs followed by the molecular docking into NMDA-GluN2B receptor, BBB
score, and the in silico toxicity evaluation. The biological activities of discovered leads on 5-HT, NE, and
DA reuptake and their effect on the NMDA-GluN2B receptor were evaluated via radio-labeled neurotransmitters
and competition radio-ligand binding experiment with [3H] ifenprodil, respectively. Lastly,
the antidepressant effect of these potential leads was determined in vivo through the forced swim test in
mice.
Results:
Two compounds were attained as potential leads after the aforementioned experiments. Further
in vitro biological evaluation identified Hit-2 as a promising lead that exerted favorable triple 5-
HT/DA/NE reuptake inhibitory activity (66.98% inhibition rate at 10 μM against hNET, 73.01% inhibition
rate at 1 μM against hDAT and 86.27% inhibition rate at 1 μM against hSERT), as well as potent
NMDA-GluN2B receptor antagonistic activity (Ki=115.73 ± 3.54 nM). The antidepressant activity of Hit-
2 was confirmed through in vivo experiments
Conclusion:
Hit-2 not only simultaneously inhibited the reuptake of 5-HT, DA, and NE, and acted as an
NMDA-GluN2B receptor antagonist in vitro but also showed in vivo antidepressant activity. These findings
may serve as a structural basis for the further development of multi-functional anti-depressive agents.
Title: Discovery of Multi-functional Lead Compounds Originating from Traditional Chinese Medicine for Developing Anti-depressive Agents via Virtual Screening
Description:
Background:
The increasing prevalence of depression has become a global health issue.
Currently
approved anti-depressive including 5-hydroxytryptamine (5-HT), dopamine (DA), norepinephrine
(NE), triple reuptake inhibitors (TRIs) and glutamate N-methyl-D-aspartate (NMDA) receptor antagonists
have limited effects because of their insufficient efficacy and/or slow onset of action.
Developing multifunctional
antidepressants that can modulate 5-HT, DA, NE, and NMDA simultaneously can potentially
overcome the current drug defects.
Objective:
This study aimed to explore leads for the development of multi-functional anti-depressive
agents that simultaneous triple reuptake inhibitory and NMDA-GluN2B receptor antagonistic activities.
Methods:
Potential leads were screened virtually from the TCMSP database based on the 3DPharmacophore
model of TRIs followed by the molecular docking into NMDA-GluN2B receptor, BBB
score, and the in silico toxicity evaluation.
The biological activities of discovered leads on 5-HT, NE, and
DA reuptake and their effect on the NMDA-GluN2B receptor were evaluated via radio-labeled neurotransmitters
and competition radio-ligand binding experiment with [3H] ifenprodil, respectively.
Lastly,
the antidepressant effect of these potential leads was determined in vivo through the forced swim test in
mice.
Results:
Two compounds were attained as potential leads after the aforementioned experiments.
Further
in vitro biological evaluation identified Hit-2 as a promising lead that exerted favorable triple 5-
HT/DA/NE reuptake inhibitory activity (66.
98% inhibition rate at 10 μM against hNET, 73.
01% inhibition
rate at 1 μM against hDAT and 86.
27% inhibition rate at 1 μM against hSERT), as well as potent
NMDA-GluN2B receptor antagonistic activity (Ki=115.
73 ± 3.
54 nM).
The antidepressant activity of Hit-
2 was confirmed through in vivo experiments
Conclusion:
Hit-2 not only simultaneously inhibited the reuptake of 5-HT, DA, and NE, and acted as an
NMDA-GluN2B receptor antagonist in vitro but also showed in vivo antidepressant activity.
These findings
may serve as a structural basis for the further development of multi-functional anti-depressive agents.
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