JoVE Journal > Behavior
Summary
Abstract
Introduction
Protocol
Results
Discussion
Disclosures
Acknowledgements
Materials
References
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Behavior

De Gedwongen Swim Test als een model van Depressieve-achtig gedrag

Published: March 02, 2015
doi:
10.3791/52587
, , ,
1School of Psychological Sciences,Tel-Aviv University, 2School of Behavioral Sciences,Academic College of Tel Aviv-Yaffo, 3Department of Education and Psychology,The Open University of Israel, 4School of Health and Life Sciences,Hadassah Academic College

Summary

This protocol describes the forced swim test, which is used for the study of depressive-like behavior in rodents. This procedure involves placing an animal in a container filled with water that eventually will lead to the exhibition of immobility behavior, which is considered to reflect behavioral despair.

Abstract

The goal of the present protocol is to describe the forced swim test (FST), which is one of the most commonly used assays for the study of depressive-like behavior in rodents. The FST is based on the assumption that when placing an animal in a container filled with water, it will first make efforts to escape but eventually will exhibit immobility that may be considered to reflect a measure of behavioral despair. This test has been extensively used because it involves the exposure of the animals to stress, which was shown to have a role in the tendency for major depression. Additionally, the FST has been shown to share some of the factors that are influenced or altered by depression in humans, including changes in food consumption, sleep abnormalities and drug-withdrawal-induced anhedonia. The main advantages of this procedure are that it is relatively easy to perform and that its results are easily and quickly analyzed. Moreover, its sensitivity to a broad range of antidepressant drugs that makes it a suitable screening test is one of the most important features leading to its high predictive validity. Despite its appeal, this model has a number of disadvantages. First, the issue of chronic augmentation is problematic in this test because in real life patients need to be treated for at least several weeks before they experience any relief from their symptoms. Last, due to the aversiveness of the FST, it is important to take into account possible influences it might have on brain structure/function if brain analyses are to be carried out following this procedure.

Introduction

Depressie is een levensbedreigende psychiatrische stoornis en een belangrijk probleem voor de volksgezondheid in de wereld met een incidentie van 5% en een prevalentie van 15-20%. Bovendien wordt geschat dat in 2020 depressie zal worden in de top drie bijdragen aan de ziektelast 1,2. Depressie wordt geassocieerd met een handicap, verminderde kwaliteit van leven, verhoogde gezondheid te hebben en als een belangrijke risicofactor voor veel ziekten, waaronder cardiovasculaire, metabole en neuropsychiatrische stoornissen 3,4 .Current farmacotherapeutische behandelingen beperkt werkzaam en zijn geassocieerd met veel schadelijke bijwerkingen 5,6. Daarom is een beter begrip van de pathofysiologie van deze aandoening samen met de ontwikkeling van innovatieve en verbeterde behandelingen blijft cruciaal. Vandaar diermodellen essentieel voor het bevorderen van onderzoek op dit gebied.

Er zijn vele modellen voor de studie van deze stoornis (<em> bv sucrose preferentie test, staart schorsing test) met de gedwongen zwemmen test (FST, ook wel bekend als Porsolt's test na de ontwikkelaar van dit model 7,8) als een van de meest gebruikte tests 7,9-12.

Tijdens de FST een dier in een bak met water waaruit niet kan ontsnappen. Het dier zal eerst proberen te ontsnappen, maar uiteindelijk zal vertonen immobiliteit (dwz drijven met de afwezigheid van enige beweging dan die welke noodzakelijk voor het houden van de neus boven water). De FST is een zeer populair model van proefdieronderzoek voor een aantal redenen. Ten eerste omvat de blootstelling van de dieren stress, die bleek een rol bij de neiging hebben voor depressie 12-14. Bovendien depressie wordt vaak gezien als een gebrek aan vermogen te behandelen met stress 15-17. Ten tweede heeft farmacologische behandeling met antidepressiva voor de proef is aangetoond dat immobiliteit verlagen de FST <sup> 18-23. Daarom wordt vaak gebruikt als een screeningstest voor nieuwe verbindingen met antidepressieve eigenschappen 15-17,24. Daarnaast is de FST aantoonbaar enkele van de factoren die worden beïnvloed of gewijzigd door depressie bij mensen, zoals veranderingen in voedselconsumptie, slaap afwijkingen en deel drugs terugtrekking geïnduceerde anhedonie 15-17,24. Dit is ook de reden waarom deze test soms gebruikt depressieve-achtig gedrag in mutante muizen, met een toename of afname in basale onbeweeglijkheid evalueren (vergelijking "wild-type" muizen) 25,26.

Protocol

OPMERKING: Alle experimentele protocollen werden goedgekeurd door het Internationale Comité voor Animal Care en gebruik in Israël. Alle inspanningen werden gedaan om het aantal gebruikte dieren en hun lijden te minimaliseren. 1. Voorbereiding van de Gedwongen Swim Test Gebruik twee aangrenzende kamers. Gebruik een kamer als een "wachtkamer" voor voorafgaande houden van de dieren aan gedragstesten, en de andere voor het uitvoeren van de procedure. Bereid trans…

Representative Results

De volgende resultaten zijn gebaseerd op ongepubliceerde gegevens uit ons laboratorium. In dit experiment werden volwassen ICR vrouwelijke muizen getest na 3 weken behandeling met de selectieve serotonine heropname remmer (SSRI) escitalopram of nieuwe kruiden anti-depressieve en anti-angst behandeling (NHT) (voor extra informatie over de kruiden-behandeling, zie 12 , 27,28). One-way ANOVA toonde dat de behandeling verlaagde depressieve-achtig gedrag in de FST [F (2,58) = 4.88, p <0.05]. Eenzijdige Dunnet a…

Discussion

FST wordt gebruikt depressieve-achtig gedrag volgen en is gebaseerd op de veronderstelling dat immobiliteit weerspiegelt een maat gedrags- wanhoop 3. De belangrijkste voordelen van deze werkwijze liggen in de relatief eenvoudige bediening en snelle resultaten. Bovendien zijn gevoeligheid voor een groot aantal antidepressiva dat het een geschikte screeningstest maakt, is een van de belangrijkste eigenschappen die tot de hoge voorspellende waarde 29. Belangrijk is, kan deze test ook onderscheid tusse…

Disclosures

The authors have nothing to disclose.

Acknowledgements

This research was supported by the Israel Science Foundation (grant No. 738/11), by the National Institute for Psychobiology in Israel (NIPI-7-2011-12), and by the Open University Foundation

Materials

Name of Material/ Equipment Company Catalog Number Comments/Description
Computer Dell intel(r) core(tm) i3-2120 cpu @ 3.30ghz, 4GB ram
Camera VIDO AU-CB422 B/W CCD CAMERA 
http://www.vido-europe.com/products_detail.asp?id=33&pcategory=2
Coding software Biobserve FST Analysis
http://www.biobserve.com/products/fst/index.html
Heating lamp Ikea AA-19025-3 ESPRESSIVIO 400.504.46 - 20W G4 Bulb 
http://www.ikea.com/ms/en_US/customer_service/assembly/E/E00050467.pdf
Heating pillow Sachs EF-188B 38*38cm Heating pillow
http://www.sachs.co.il/eng/lego_tree.php?instance_id=21&actions=show&id=
604
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References

  1. Levinson, D. F. The genetics of depression: a review. Biological psychiatry. 60, 84-92 (2006).
  2. Murray, C. J., Lopez, A. D. Alternative projections of mortality and disability by cause 1990-2020: Global Burden of Disease Study. Lancet. 349, 1498-1504 (1997).
  3. Cryan, J. F., Holmes, A. The ascent of mouse: advances in modelling human depression and anxiety. Nature reviews. Drug discovery. 4, 775-790 (2005).
  4. Thase, M. E. Managing depressive and anxiety disorders with escitalopram. Expert opinion on pharmacotherapy. 7, 429-440 (2006).
  5. Lam, R. W., Kennedy, S. H. Evidence-based strategies for achieving and sustaining full remission in depression: focus on metaanalyses. Canadian journal of psychiatry. Revue canadienne de psychiatrie. 49, 17S-26S (2004).
  6. Dording, C. M., et al. The pharmacologic management of SSRI-induced side effects: a survey of psychiatrists. Annals of clinical psychiatry : official journal of the American Academy of Clinical Psychiatrists. 14, 143-147 (2002).
  7. Porsolt, R. D., Le Pichon, M., Jalfre, M. Depression: a new animal model sensitive to antidepressant treatments. Nature. 266, 730-732 (1977).
  8. Porsolt, R. D., Bertin, A., Jalfre, M. Behavioral despair in mice: a primary screening test for antidepressants. Archives internationales de pharmacodynamie et de therapie. 229, 327-336 (1977).
  9. Cryan, J. F., Markou, A., Lucki, I. Assessing antidepressant activity in rodents: Recent developments and future needs. Trends in Pharmacological Sciences. 23, 238-245 (2002).
  10. Cryan, J. F., et al. Norepinephrine-deficient mice lack responses to antidepressant drugs, including selective serotonin reuptake inhibitors. Proceedings of the National Academy of Sciences of the United States of America. 101, 8186-8191 (2004).
  11. Porsolt, R. D., Anton, G., Blavet, N., Jalfre, M. Behavioural despair in rats: A new model sensitive to antidepressant treatments. European Journal of Pharmacology. 47, 379-391 (1978).
  12. Doron, R., et al. A novel herbal treatment reduces depressive-like behaviors and increases BDNF levels in the brain of stressed mice. Life sciences. 94, 151-157 (2014).
  13. Caspi, A., et al. Influence of life stress on depression: Moderation by a polymorphism in the 5-HTT gene. Science. 301, 386-389 (2003).
  14. Kaufman, J., et al. Brain-derived neurotrophic factor-5-HTTLPR gene interactions and environmental modifiers of depression in children. Biological psychiatry. 59, 673-680 (2006).
  15. Anisman, H., Zacharko, R. M. Multiple neurochemical and behavioral consequences of stressors: Implications for depression. Pharmacology and Therapeutics. 46, 119-136 (1990).
  16. Kessler, R. C. The effects of stressful life events on depression. Annual Review of Psychology. 48, 191-214 (1997).
  17. Sullivan, P. F., Neale, M. C., Kendler, K. S. Genetic epidemiology of major depression: Review and meta-analysis. American Journal of Psychiatry. 157, 1552-1562 (2000).
  18. Cryan, J. F., Valentino, R. J., Lucki, I. Assessing substrates underlying the behavioral effects of antidepressants using the modified rat forced swimming test. Neuroscience and biobehavioral reviews. 29, 547-569 (2005).
  19. Detke, M. J., Lucki, I. Detection of serotonergic and noradrenergic antidepressants in the rat forced swimming test: The effects of water depth. Behavioural Brain Research. 73, 43-46 (1996).
  20. Hemby, S. E., et al. Potential antidepressant effects of novel tropane compounds, selective for serotonin or dopamine transporters. Journal of Pharmacology and Experimental Therapeutics. 282, 727-733 (1997).
  21. Bouvard, M., Stinus, L. In the rat forced swimming test, chronic but not subacute administration of dual 5-HT/NA antidepressant treatments may produce greater effects than selective drugs. Behavioural Brain Research. 136, 521-532 (2002).
  22. Page, M. E., Detke, M. J., Dalvi, A., Kirby, L. G., Lucki, I. Serotonergic mediation of the effects of fluoxetine, but not desipramine, in the rat forced swimming test. Psychopharmacology. 147, 162-167 (1999).
  23. Rubalcava, C., Lucki, I. Strain differences in the behavioral effects of antidepressant drugs in the rat forced swimming test. Neuropsychopharmacology. 22, 191-199 (2000).
  24. Cryan, J. F., Mombereau, C., Vassout, A. The tail suspension test as a model for assessing antidepressant activity: Review of pharmacological and genetic studies in mice. Neuroscience and biobehavioral reviews. 29, 571-625 (2005).
  25. Cryan, J. F., Mombereau, C. In search of a depressed mouse: Utility of models for studying depression-related behavior in genetically modified mice. Molecular Psychiatry. 9, 326-357 (2004).
  26. Sang, K. P., et al. Par-4 links dopamine signaling and depression. Cell. 122, 275-287 (2005).
  27. Doron, R., et al. Anxiolytic effects of a novel herbal treatment in mice models of anxiety. Life sciences. 90, 995-1000 (2012).
  28. Doron, R., et al. Escitalopram or novel herbal mixture treatments during or following exposure to stress reduce anxiety-like behavior through corticosterone and BDNF modifications. PloS one. 9, e91455 (2014).
  29. Borsini, F., Meli, A. Is the forced swimming test a suitable model for revealing antidepressant activity. Psychopharmacology. 94, 147-160 (1988).
  30. Reinhold, J. A., Mandos, L. A., Rickels, K., Lohoff, F. W. Pharmacological treatment of generalized anxiety disorder. Expert opinion on pharmacotherapy. 12, 2457-2467 (2011).
  31. Estrada-Camarena, E., Fernandez-Guasti, A., Lopez-Rubalcava, C. Interaction between estrogens and antidepressants in the forced swimming test in rats. Psychopharmacology. 173, 139-145 (2004).
  32. Weiss, J. M., Kilts, C. D. Animal models of depression and schizophrenia. Textbook of Psychopharmacology. , 89-131 (1998).
  33. Armario, A., Gavaldà, A., Martí, J. Comparison of the behavioural and endocrine response to forced swimming stress in five inbred strains of rats. Psychoneuroendocrinology. 20, 879-890 (1995).
  34. Paré, W. P. Open field, learned helplessness, conditioned defensive burying, and forced-swim tests in WKY rats. Physiology and Behavior. 55, 433-439 (1994).
  35. Overstreet, D. H., Friedman, E., Mathe, A. A., Yadid, G. The Flinders Sensitive Line rat: a selectively bred putative animal model of depression. Neuroscience and biobehavioral reviews. 29, 739-759 (2005).
  36. Piras, G., Piludu, M. A., Giorgi, O., Corda, M. G. Effects of chronic antidepressant treatments in a putative genetic model of vulnerability (Roman low-avoidance rats) and resistance (Roman high-avoidance rats) to stress-induced depression. Psychopharmacology. 231, 43-53 (2014).
  37. Bielajew, C., et al. Strain and Gender Specific Effects in the Forced Swim Test. Effects of Previous Stress Exposure. Stress. 6, 269-280 (2003).
  38. Fujisaki, C., et al. An immnosuppressive drug, cyclosporine-A acts like anti-depressant for rats under unpredictable chronic stress. Journal of Medical and Dental Sciences. 50, 93-100 (2003).
  39. Gomez, R., Vargas, C. R., Wajner, M., Barros, H. M. T. Lower in vivo brain extracellular GABA concentration in diabetic rats during forced swimming. Brain research. 968, 281-284 (2003).
  40. Hilakivi-Clarke, L. A., Wozniak, K. M., Durcan, M. J., Linnoila, M. Behavior of streptozotocin-diabetic mice in tests of exploration, locomotion, anxiety, depression and aggression. Physiology and Behavior. 48, 429-433 (1990).
  41. Cryan, J. F., Hoyer, D., Markou, A. Withdrawal from chronic amphetamine induces depressive-like behavioral effects in rodents. Biological psychiatry. 54, 49-58 (2003).
  42. Portella, M. J., et al. Can we really accelerate and enhance the selective serotonin reuptake inhibitor antidepressant effect? A randomized clinical trial and a meta-analysis of pindolol in nonresistant depression. The Journal of clinical psychiatry. 72, 962-969 (2011).
  43. Machado-Vieira, R., Salvadore, G., Luckenbaugh, D. A., Manji, H. K., Zarate, C. A. Rapid onset of antidepressant action: a new paradigm in the research and treatment of major depressive disorder. The Journal of clinical psychiatry. 69, 946-958 (2008).
  44. Bordet, R., Thomas, P., Dupuis, B. Effect of pindolol on onset of action of paroxetine in the treatment of major depression: intermediate analysis of a double-blind, placebo-controlled trial. Reseau de Recherche et d’Experimentation Psychopharmacologique. The American journal of psychiatry. 155, 1346-1351 (1998).
  45. Dulawa, S. C., Holick, K. A., Gundersen, B., Hen, R. Effects of chronic fluoxetine in animal models of anxiety and depression. Neuropsychopharmacology. 29, 1321-1330 (2004).
  46. Willner, P. Animal models of depression: An overview. Pharmacology and Therapeutics. 45, 425-455 (1990).
  47. Jefferys, D., Funder, J. The effect of water temperature on immobility in the forced swimming test in rats. European Journal of Pharmacology. 253, 91-94 (1994).
  48. West, A. P. Neurobehavioral studies of forced swimming: The role of learning and memory in the forced swim test. Progress in Neuro-Psychopharmacology and Biological Psychiatry. 14, 863-877 (1990).
  49. De Pablo, J. M., Parra, A., Segovia, S., Guillamon, A. Learned immobility explains the behavior of rats in the forced swimming test. Physiology and Behavior. 46, 229-237 (1989).
  50. Dal-Zotto, S., Martí, O., Armario, A. Influence of single or repeated experience of rats with forced swimming on behavioural and physiological responses to the stressor. Behavioural Brain Research. 114, 175-181 (2000).
  51. Rittenhouse, P. A., López-Rubalcava, C., Stanwood, G. D., Lucki, I. Amplified behavioral and endocrine responses to forced swim stress in the Wistar-Kyoto rat. Psychoneuroendocrinology. 27, 303-318 (2002).
  52. Overstreet, D. H., Keeney, A., Hogg, S. Antidepressant effects of citalopram and CRF receptor antagonist CP-154,526 in a rat model of depression. European Journal of Pharmacology. 492, 195-201 (2004).
  53. Chaki, S., et al. MGS0039: A potent and selective group II metabotropic glutamate receptor antagonist with antidepressant-like activity. Neuropharmacology. 46, 457-467 (2004).
  54. Mague, S. D., et al. Antidepressant-like effects of κ-opioid receptor antagonists in the forced swim test in rats. Journal of Pharmacology and Experimental Therapeutics. 305, 323-330 (2003).
  55. Molina-Hernández, M., Téllez-Alcántara, N. P. Antidepressant-like actions of pregnancy, and progesterone in Wistar rats forced to swim. Psychoneuroendocrinology. 26, 479-491 (2001).
  56. Estrada-Camarena, E., Fernández-Guasti, A., López-Rubalcava, C. Antidepressant-like effect of different estrogenic compounds in the forced swimming test. Neuropsychopharmacology : official publication of the American College of Neuropsychopharmacology. 28, 830-838 (2003).
  57. Gersner, R., Gordon-Kiwkowitz, M., Zangen, A. Automated behavioral analysis of limbs’ activity in the forced swim test. Journal of neuroscience. 180, 82-86 (2009).
  58. Einat, H. Partial effects of the protein kinase C inhibitor chelerythrine in a battery of tests for manic-like behavior in black Swiss mice. Pharmacological reports : PR. 66, 722-725 (2014).

Tags

Forced Swim TestDepressive-like BehaviorRodent ModelBehavioral DespairStressAntidepressant DrugsPredictive ValidityChronic AugmentationBrain Structure/function

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Yankelevitch-Yahav, R., Franko, M., Huly, A., Doron, R. The Forced Swim Test as a Model of Depressive-like Behavior. J. Vis. Exp. (97), e52587, doi:10.3791/52587 (2015).
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