| Literature DB >> 29118373 |
Trevor J Hamilton1,2, Adam Morrill3, Kayla Lucas3, Joshua Gallup3, Megan Harris3, Meghan Healey3, Taylor Pitman3, Melike Schalomon3, Shannon Digweed3, Martin Tresguerres4.
Abstract
Scopolamine (hyoscine) is a muscarinic acetylcholine receptor antagonist that has traditionally been used to treat motion sickness in humans. However, studies investigating depressed and bipolar populations have found that scopolamine is also effective at reducing depression and anxiety symptoms. The potential anxiety-reducing (anxiolytic) effects of scopolamine could have great clinical implications for humans; however, rats and mice administered scopolamine showed increased anxiety in standard behavioural tests. This is in direct contrast to findings in humans, and complicates studies to elucidate the specific mechanisms of scopolamine action. The aim of this study was to assess the suitability of zebrafish as a model system to test anxiety-like compounds using scopolamine. Similar to humans, scopolamine acted as an anxiolytic in individual behavioural tests (novel approach test and novel tank diving test). The anxiolytic effect of scopolamine was dose dependent and biphasic, reaching maximum effect at 800 µM. Scopolamine (800 µM) also had an anxiolytic effect in a group behavioural test, as it significantly decreased their tendency to shoal. These results establish zebrafish as a model organism for studying the anxiolytic effects of scopolamine, its mechanisms of action and side effects.Entities:
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Year: 2017 PMID: 29118373 PMCID: PMC5678162 DOI: 10.1038/s41598-017-15374-w
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379
Figure 1Ethanol decreases anxiety in the novel approach test. (a) Trackplot of an individual control zebrafish behaviour in the 5 minute trial. (b) Trackplot of an individual zebrafish exposed to 1.5% ethanol. (c) Heatmap (coloured representation of zebrafish location over the trial) for the same fish shown in (a). (d) Heatmap for the same fish shown in (b). (e) Time fish spent in the inner zone containing the novel object for different doses of ethanol. **P < 0.01, Kruskal-Wallis test with Dunn’s multiple comparison post hoc test.
Distance traveled and immobility for control and ethanol-dosed zebrafish in the novel approach test.
| Distance Travelled (cm) | Immobility (s) | |
|---|---|---|
| Control (n = 18) | 3673 ± 234.7 | 16.06 ± 7.677 |
| 0.5% Ethanol (n = 16) | 3231 ± 175.7 | 3.827 ± 3.048 |
| 1.0% Ethanol (n = 15) | 2793 ± 561.3 | 22.70 ± 16.09 |
| 1.5% Ethanol (n = 18) | 2647 ± 339.7 | 76.46 ± 22.63** |
There was a significant difference between controls and 1.5% ethanol for immobility (**P < 0.01) (Kruskal-Wallis test with Dunn’s multiple comparison post hoc test).
Figure 2Scopolamine decreases anxiety in the novel approach test. (a) Trackplot of an individual control zebrafish behaviour in the 5 minute trial. (b) Trackplot of an individual zebrafish exposed to 800 μM scopolamine. (c) Heatmap (coloured representation of zebrafish location over the trial) for the same fish shown in (a). (d) Heatmap for the same fish shown in (b). (e) Time fish spent in the inner zone containing the novel object for different doses of scopolamine. **P < 0.01, Kruskal-Wallis test with Dunn’s multiple comparison post hoc test.
Distance traveled and immobility for control and scopolamine-dosed zebrafish in the novel approach test.
| Distance travelled (cm) | Immobility (s) | |
|---|---|---|
| Control (n = 18) | 3673 ± 234.7 | 16.06 ± 7.677 |
| 200 µM scopolamine(n = 18) | 4115 ± 228.4 | 6.742 ± 3.137 |
| 400 µM scopolamine (n = 16) | 3738 ± 287.2 | 1.403 ± 0.8007 |
| 800 µM scopolamine (n = 19) | 3926 ± 377.6 | 8.051 ± 3.78 |
| 1200 µM scopolamine (n = 16) | 2855 ± 183.1 | 4.023 ± 2.275 |
| 1600 µM scopolamine (n = 18) | 3821 ± 263.1 | 10.08 ± 6.647 |
There were no significant differences between controls and scopolamine for distance travelled and immobility for all scopolamine doses.
Figure 3Scopolamine decreases anxiety in the novel tank diving test. (a) Heatmap of an individual control zebrafish behaviour in the 10 minute trial. (b) Heatmap of an individual zebrafish exposed to 800 μM scopolamine. (c) Time fish spent in each zone for an 800 μM dose of scopolamine (red bars) compared to controls (black bars). *P < 0.05, unpaired t-test.
Figure 4Scopolamine decreases anxiety in a test of group behaviour. (a) Trackplot of a group of 6 control zebrafish for the first 30 seconds of the trial. Each coloured line represents an individual fish. (b) Trackplot of a group of 6 zebrafish dosed with 800 μM scopolamine. (c) Scopolamine (800 μM) increased the inter-individual distance in groups of zebrafish. (d) Scopolamine (800 μM) increased the nearest neighbour distance in groups of zebrafish. *P < 0.05, ****P < 0.0001, unpaired t-test.