| Literature DB >> 22619570 |
Noah S Philip1, Linda L Carpenter, Audrey R Tyrka, Lawrence H Price.
Abstract
An important new area of antidepressant drug development involves targeting the nicotinic acetylcholine receptor (nAChR). This receptor, which is distributed widely in regions of the brain associated with depression, is also implicated in other important processes that are relevant to depression, such as stress and inflammation. The two classes of drugs that target nAChRs can be broadly divided into mecamylamine- and cytisine-based compounds. These drugs probably exert their effects via antagonism at α4β2 nAChRs, and strong preclinical data support the antidepressant efficacy of both classes when used in conjunction with other primary antidepressants (e.g., monoamine reuptake inhibitors). Although clinical data remain limited, preliminary results in this area constitute a compelling argument for further evaluation of the nAChR as a target for future antidepressant drug development.Entities:
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Year: 2012 PMID: 22619570 PMCID: PMC3349306 DOI: 10.1100/2012/104105
Source DB: PubMed Journal: ScientificWorldJournal ISSN: 1537-744X
Evidence for MEC/S-MEC in mouse models of depression.
| Study | Compound(s) | MEC/s-MEC dose | Results |
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| Popik et al. [ | MEC + CTP | 0.025 mg/kg | Improved FST |
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| Rabenstein et al. [ | MEC | 1 mg/kg | Improved FST and TST |
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Caldarone et al. [ | MEC | 0.50, 0.75, or 1.0 mg/kg | Improved FST/TST |
| MEC + AMI | Further improved FST/TST | ||
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| Andreasen et al. [ | MEC | 3 or 10 mg/kga | Improved FST/TST |
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Andreasen and Redrobe [ | MEC + CTP | 1, 3 mg/kg | No effect on FST/TST |
| MEC + REB | |||
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| Mineur et al. [ | MEC | 1 mg/kg | Improved FST/TST |
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| Lippiello et al. [ | S-MEC | 3 mg/kg | Improved FST |
Notes: a1–10 mg/kg doses tested, and only doses at 3 and 10 mg/kg with improved FST/TST.
Abbreviations: MEC: mecamylamine; CTP: citalopram; IMI: imipramine; AMI: amitriptyline: REB: reboxetine; S-MEC: s-mecamylamine; FST: forced swim test; TST: tail suspension test.
Evidence for cytisine and cytisine-based compounds in mouse models of depression.
| Study | Compound(s) | CYT-compound dose | Results |
|---|---|---|---|
| Mineur et al. [ | CYT | 1.5 mg/kga | Improved FST/TST |
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Mineur et al. [ | CYT | 1, 1.5 mg/kg | Improved FST/TST |
| 3-pyr-CYT | Improved FST/TST | ||
| 5-Br-CYT | No effect on FST/TSTb | ||
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Rollema et al. [ | VNCL | 0.178, 0.56, 1, 1.78, 3.2, 5.6 mg/kg | Improved FST |
| VNCL + SERT | 0.56, 5.6 mg/kg | Improved FSTc | |
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| Kozikowski et al. [ | SAZ-A | 1 mg/kg | Improved FST |
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Turner et al. [ | VNCL | 0.01, 0.1, 1 mg/kg | No effect on FST |
| SAZ-A | 1 mg/kg | Improved FSTd | |
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Caldarone et al. [ | VNCL | 0.3, 1, and 3 mg/kg | Improved FST |
| SAZ-A | 1, 3, and 10 mg/kg | Improved FST | |
Notes: a0.2, 0.6, 1.0, and 1.5 mg/kg CYT tested.
bNo CNS penetration.
cLow dose VNCL (0.56 mg/kg) combined with low dose SERT (1.78 mg/kg) produced no significant effect on FST performance.
dSAZ-A at doses of 0.05–0.5 mg/kg had no effect on FST performance.
Abbreviations: CYT: cytisine; 3-pyr-CYT: 3-[pyridin-3′-yl]-cytisine; 5-Br-CYT: 5-bromo-cytisine; VNCL: varenicline; SERT: sertraline; SAZ-A: sazetidine-A; FST: forced swim test; TST: tail suspension test.