Potential antidepressant effect of amantadine: a review of preclinical studies and clinical trials

Raupp-Barcaro, Inara F.; Vital, Maria A.; Galduróz, José C.; Andreatini, Roberto

doi:10.1590/1516-4446-2017-2393

Inara F. Raupp-Barcaro

Departamento de Farmacologia, Setor de Ciências Biológicas, Universidade Federal do Paraná, Curitiba, PR, Brazil

Maria A. Vital

Departamento de Farmacologia, Setor de Ciências Biológicas, Universidade Federal do Paraná, Curitiba, PR, Brazil

José C. Galduróz

Departamento de Psicobiologia, Universidade Federal de São Paulo, São Paulo, SP, Brazil

Roberto Andreatini Correspondence: Roberto Andreatini, Laboratório de Fisiologia e Farmacologia do Sistema Nervoso Central, Departamento de Farmacologia, Universidade Federal do Paraná, Centro Politécnico, Jardim das Américas, CEP 81540-990, Caixa Postal 19031, Curitiba, PR, Brazil. E-mail: randreatini@ufpr.br

Departamento de Farmacologia, Setor de Ciências Biológicas, Universidade Federal do Paraná, Curitiba, PR, Brazil

Correspondence: Roberto Andreatini, Laboratório de Fisiologia e Farmacologia do Sistema Nervoso Central, Departamento de Farmacologia, Universidade Federal do Paraná, Centro Politécnico, Jardim das Américas, CEP 81540-990, Caixa Postal 19031, Curitiba, PR, Brazil. E-mail: randreatini@ufpr.br

Disclosure The authors report no conflicts of interest.

Dopaminergic system	Amantadine acts on the presynaptic membrane, enhancing dopamine release¹⁴14. Scatton B, Cheramy A, Besson MJ, Glowinski J. Increased synthesis and release of dopamine in the striatum of the rat after amantadine treatment. Eur J Pharmacol. 1970;13:131-3.,¹⁵15. Von Voigtlander PF, Moore KE. Dopamine: release from the brain in vivo by amantadine. Science. 1971;174:408-10. and inhibiting its reuptake in brain homogenates at higher doses.¹⁶16. Fletcher EA, Redfern PH. The effect of amantadine on the uptake of dopamine and noradrenaline by rat brain homogenates. J Pharm Pharmacol. 1970;22:957-9.,¹⁷17. Heimans RL, Rand MJ, Fennessy MR. Effects of amantadine on uptake and release of dopamine by a particulate fraction of rat basal ganglia. J Pharm Pharmacol. 1972;24:875-9. Several of these dopaminergic effects are seen at concentrations higher than those that are used clinically in humans.¹⁸18. Baldessarini RJ, Lipinski JF, Chace KV. Effects of amantadine hydrochloride on catecholamine metabolism in the brain of the rat. Biochem Pharmacol. 1972;21:77-87. 19. Heikkila RE, Cohen G. Evaluation of amantadine as a releasing agent or uptake blocker for H3-dopamine in rat brain slices. Eur J Pharmacol. 1972;20:156-60.-²⁰20. Stone TW. Responses of neurones in the cerebral cortex and caudate nucleus to amantadine, amphetamine and dopamine. Br J Pharmacol. 1976;56:101-10. The effects of amantadine on dopaminergic transmission are still debatable. Some results show that amantadine has a direct action on D₂ receptors,²⁰20. Stone TW. Responses of neurones in the cerebral cortex and caudate nucleus to amantadine, amphetamine and dopamine. Br J Pharmacol. 1976;56:101-10. 21. Maj J, Sowińska H, Baran L. The effect of amantadine on motor activity and catalepsy in rats. Psychopharmacologia. 1972;24:296-307.-²²22. Chopra YM, Dandiya PC. Potentiation of anticatatonic effect of antidepressants by amantadine. Indian J Med Res. 1977;66:142-9. but other studies have reported no significant actions on catecholaminergic receptors.²³23. Stromberg U, Svensson TH, Waldeck B. On the mode of action of amantadine. J Pharm Pharmacol. 1970;22:959-62. 24. Farnebo LO, Fuxe K, Goldstein M, Hamberger B, Ungerstedt U. Dopamine and noradrenaline releasing action of amantadine in the central and peripheral nervous system: a possible mode of action in Parkinson's disease. Eur J Pharmacol. 1971;16:27-38.-²⁵25. Henkel JG, Hane JT, Gianutsos G. Structure-anti-Parkinson activity relationships in the aminoadamantanes. Influence of bridgehead substitution. J Med Chem. 1982;25:51-6. Moresco et al.²⁶26. Moresco RM, Volonte MA, Messa C, Gobbo C, Galli L, Carpinelli A, et al. New perspectives on neurochemical effects of amantadine in the brain of parkinsonian patients: a PET – [11C]raclopride study. J Neural Transm (Vienna). 2002;109:1265-74. evaluated patients who received amantadine (200 mg/day, 10-14 days) and were being treated with L-DOPA, which was suspended the night before positron emission tomography scans were performed. The patients were free from dopaminergic agonists, anticholinergics, and antidepressants. The patients presented an increase in [¹¹11. Hubsher G, Haider M, Okun MS. Amantadine: the journey from fighting flu to treating Parkinson disease. Neurology. 2012;78:1096-9.C]raclopride binding in the caudate and putamen. This suggests that amantadine increases the neosynthesis of D₂ receptors, which may represent one mechanism of action. The effects of amantadine are also related to the inhibition of dopamine reuptake. Its antiparkinsonian activity may be attributable to the inhibition of dopamine reuptake into presynaptic neurons or an increase in dopamine release from presynaptic fibers.²⁷27. Cacabelos R. Parkinson's disease: from pathogenesis to pharmacogenomics. Int J Mol Sci. 2017;18(3). doi: 10.3390/ijms18030551. 10.3390/ijms18030551...
Noradrenergic system	Amantadine appears to have pharmacological actions that are similar to those of tricyclic antidepressants.¹⁰10. Huber TJ, Dietrich DE, Emrich HM. Possible use of amantadine in depression. Pharmacopsychiatry. 1999;32:47-55. A significant increase in norepinephrine levels was observed after an oral dose of amantadine in healthy subjects.²⁸28. Lechin F, van der Dijs B, Pardey-Maldonado B, Rivera JE, Baez S, Lechin ME. Effects of amantadine on circulating neurotransmitters in healthy subjects. J Neural Transm (Vienna). 2010;117:293-9. Noradrenergic mechanisms may also be involved in the actions of amantadine.²⁹29. Moryl E, Danysz W, Quack G. Potential antidepressive properties of amantadine, memantine and bifemelane. Pharmacol Toxicol. 1993;72:394-7.,³⁰30. Dutta A, McKie S, Deakin JF. Ketamine and other potential glutamate antidepressants. Psychiatry Res. 2015;225:1-13.
Glutamatergic system	Amantadine is an N-methyl-D-aspartate (NMDA) receptor antagonist that is commonly used for the treatment of Parkinson’s disease. It is thought to inhibit NMDA receptor activation through the stabilization of ion channels and more rapid channel closure.³⁰30. Dutta A, McKie S, Deakin JF. Ketamine and other potential glutamate antidepressants. Psychiatry Res. 2015;225:1-13.,³¹31. Blanpied TA, Clarke RJ, Johnson JW. Amantadine inhibits NMDA receptors by accelerating channel closure during channel block. J Neurosci. 2005;25:3312-22.
Immunomodulation	Amantadine may also have immunomodulatory properties. It restored the production of interleukin (IL)-2, which is dysfunctional in Parkinson’s disease patients.³²32. Wandinger KP, Hagenah JM, Klüter H, Rothermundt M, Peters M, Vieregge P. Effects of amantadine treatment on in vitro production of interleukin-2 in de-novo patients with idiopathic Parkinson's disease. J Neuroimmunol. 1999;98:214-20.,³³33. Warren N, Burn DJ. The use of amantadine in Parkinson’s disease and other akinetic-rigid disorders. Adv Clin Neurosci Rehabil. 2004;4:38-41. IL-2 levels did not correspond to clinical improvement, so the significance of these findings is unclear. Other studies³³33. Warren N, Burn DJ. The use of amantadine in Parkinson’s disease and other akinetic-rigid disorders. Adv Clin Neurosci Rehabil. 2004;4:38-41.,³⁴34. Uitti RJ, Rajput AH, Ahlskog JE, Offord KP, Schroeder DR, Ho MM, et al. Amantadine treatment is an independent predictor of improved survival in Parkinson's disease. Neurology. 1996;46:1551-6. showed that amantadine treatment was an independent predictor of improved survival in Parkinson’s disease.

Reference	Animal	Amantadine effective dose(mg/kg)^* * Doses in parentheses were ineffective.	Treatment(route)	Depression induction	Animal model	Results	Conclusion
FST
Moryl et al.²⁹29. Moryl E, Danysz W, Quack G. Potential antidepressive properties of amantadine, memantine and bifemelane. Pharmacol Toxicol. 1993;72:394-7.	Rat (male)	20, 40, 80	Acute (i.p.)		FST	FST: ↓ immobility time Locomotor activity (OFT): ↓ ambulation, peeping, rearing, and walking time	Antidepressant-like effects
Rogoz et al.³⁷37. Rogóz Z, Skuza G, Maj J, Danysz W. Synergistic effect of uncompetitive NMDA receptor antagonists and antidepressant drugs in the forced swimming test in rats. Neuropharmacology. 2002;42:1024-30.	Rat (male)	(10), 20	Acute (i.p.)		FST	FST: ↓ immobility time Locomotor activity (OFT): no effect	Antidepressant-like effects
Rogoz, et al.³⁸38. Rogóz Z, Skuza G, Kusmider M, Wójcikowski J, Kot M, Daniel WA. Synergistic effect of imipramine and amantadine in the forced swimming test in rats. Behavioral and pharmacokinetic studies. Pol J Pharmacol. 2004;56:179-85.	Rat (male)	(10), 20	Acute (i.p.)		FST	FST: ↓ immobility time Locomotor activity (OFT): no effect	Antidepressant-like effects
CUMS
Yu et al.⁴³43. Yu M, Zhang Y, Chen X, Zhang T. Antidepressant-like effects and possible mechanisms of amantadine on cognitive and synaptic deficits in a rat model of chronic stress. Stress. 2016;19:104-13.	Rat (male)	25	Chronic (oral)	CUMS	SPTMWMBody weight loss	SPT: ↑ sucrose consumption MWM: ↓ escape latency Body weight loss: prevented Locomotor activity (swim velocity in MWM): no effect	Antidepressant-like effects
Reserpine syndrome
Maj et al.²¹21. Maj J, Sowińska H, Baran L. The effect of amantadine on motor activity and catalepsy in rats. Psychopharmacologia. 1972;24:296-307.	Rat (male and female)	(20), 40, 80	Acute (i.p.)	Reserpine 5 mg/kg	Locomotor activity Catalepsy	↓ reserpine-induced hypolocomotion ↓ catalepsy Locomotor activity (AA): no effect	Antidepressant-like effects
Jurna et al.⁴⁴44. Jurna I, Grossmann W, Nell T. Depression by amantadine of drug-induced rigidity in the rat. Neuropharmacology. 1972;11:559-64.	Rat (unspecified sex)	50	Acute (i.v.)	Reserpine 10 mg/kg	Electromyography	↓ muscle rigidity Locomotor activity: NE	Antidepressant-like effects
Lassen⁴⁵45. Lassen JB. The effect of amantadine and (+)-amphetamine on motility in rats after inhibition of monoamine synthesis and storage. Psychopharmacologia. 1973;29:55-64.	Rats (female)	25, 50	Acute (s.c.)	Reserpine 7.5 mg/kg	Locomotor activity	Did not affect reserpine-induced hypolocomotion AA: ↑ locomotor activity	Ineffective
Colpaert et al.⁴⁶46. Colpaert FC. Pharmacological characteristics of tremor, rigidity and hypokinesia induced by reserpine in rat. Neuropharmacology. 1987;26:1431-40.	Rats (female)	24-110 (ED₅₀)	Acute (oral)	Reserpine 40 mg/kg	Hypokinesia Catalepsy	Prevented reserpine-induced hypokinesia ↓ catalepsy Locomotor activity: NE	Antidepressant-like effects
Goldstein et al.⁴⁷47. Goldstein JM, Barnett A, Malick JB. The evaluation of anti-Parkinson drugs on reserpine-induced rigidity in rats. Eur J Pharmacol. 1975;33:183-8.	Rats (male)	21.8 (ED₅₀)	Acute (s.c.)	Reserpine 5 mg/kg	Reserpine-induced hindlimb rigidity	Prevented reserpine-induced rigidity Locomotor activity: NE	Antidepressant-like effects
Cox & Tha⁴⁸48. Cox B, Tha SJ. The role of dopamine and noradrenaline in temperature control of normal and reserpine-pretreated mice. J Pharm Pharmacol. 1975;27:242-7.	Mouse (male and female)	(25)	Acute (i.p.)	Reserpine 5 mg/kg	Reserpine-induced hypothermia	No effect Locomotor activity: NE	Ineffective
Messiha⁴⁹49. Messiha FS. Effect of amantadine on chlorpromazine and reserpine-induced behavioral depression in the mouse. Neurosci Biobehav Rev. 1988;12:219-22.	Mouse (male)	100	Acute (i.p.)	Reserpine 0.2 mg/kg	Locomotor activity	↑ reserpine-induced hypolocomotion Locomotor activity (AA): ↓	Ineffective
Moryl et al.²⁹29. Moryl E, Danysz W, Quack G. Potential antidepressive properties of amantadine, memantine and bifemelane. Pharmacol Toxicol. 1993;72:394-7.	Mouse (male)	(20), 40, 80	Acute (i.p.)	Reserpine 2.5 mg/kg	Hypothermia	↓ reserpine-induced hypothermia Locomotor activity: NE (for mice)	Antidepressant-like effects
Comorbidity
Tan et al.⁵⁰50. Tan L, Ge H, Tang J, Fu C, Duanmu W, Chen Y, et al. Amantadine preserves dopamine level and attenuates depression-like behavior induced by traumatic brain injury in rats. Behav Brain Res. 2015;279:274-82.	Rat (male)	45-135	Chronic (28 days) (i.p.)	Depressive-like behavior induced by traumatic brain injury	SPTFST	SPT: ↑ sucrose preference FST: ↓ immobility time Locomotor activity: NE	Antidepressant-like effects
Co-administration
Skuza & Rogóz³⁹39. Skuza G, Rogóz Z. Effect of combined treatment with selective σ ligands and amantadine in the forced swimming test in rats. Pol J Pharmacol. 2002;54:699-702.	Rat (male)	(10)	Acute (i.p.)	+ σ₁ receptor agonist SA4503 or σ₂ receptor agonist siramesine	FST	FST: ↓ immobility time Locomotor activity (AA): no effect	Potentiated antidepressant-like effects of σ receptor agonists
Rogoz et al.³⁷37. Rogóz Z, Skuza G, Maj J, Danysz W. Synergistic effect of uncompetitive NMDA receptor antagonists and antidepressant drugs in the forced swimming test in rats. Neuropharmacology. 2002;42:1024-30.	Rat (male)	(10)	Acute (i.p.)	+ venlafaxine, imipramine, or fluoxetine	FST	FST: ↓ immobility time Locomotor activity (OFT): no effect or ↓ locomotor activity	Potentiated antidepressant-like effects
Rogoz et al.³⁸38. Rogóz Z, Skuza G, Kusmider M, Wójcikowski J, Kot M, Daniel WA. Synergistic effect of imipramine and amantadine in the forced swimming test in rats. Behavioral and pharmacokinetic studies. Pol J Pharmacol. 2004;56:179-85.	Rat (male)	20	Acute (i.p.)	+ imipramine	FST	FST: ↓ immobility time Locomotor activity (OFT): ↓ locomotor activity	Potentiated antidepressant-like effects
Kubera et al.⁵¹51. Kubera M, Basta-Kaim A, Budziszewska B, Rogóz Z, Skuza G, Leskiewicz M, et al. Effect of amantadine and imipramine on immunological parameters of rats subjected to a forced swimming test. Int J Neuropsychopharmacol. 2006;9:297-305.	Rat (male)	(10)	Acute (i.p.)	+ imipramine	FST	FST: ↓ immobility time Locomotor activity: NE	Potentiated antidepressant-like effects
Skuza & Rogóz⁴⁰40. Skuza G, Rogóz Z. The synergistic effect of selective sigma receptor agonists and uncompetitive NMDA receptor antagonists in the forced swimming test in rats. J Physiol Pharmacol. 2006;57:217-29.	Rat (male)	(10)	Acute (i.p.)	+ σ₁ receptor agonist SA4503	FST	FST: ↓ immobility time Locomotor activity (AA): no effect	Potentiated antidepressant-like effects of σ₁ receptor agonist
Rogóz et al.⁴¹41. Rogóz Z, Kubera M, Rogóz K, Basta-Kaim A, Budziszewska B. Effect of co-administration of fluoxetine and amantadine on immunoendocrine parameters in rats subjected to a forced swimming test. Pharmacol Rep. 2009;61:1050-60.	Rat (male)	(10)	Acute (i.p.)	+ fluoxetine	FST	FST: ↓ immobility time Locomotor activity: NE	Potentiated antidepressant-like effects of fluoxetine
Skuza et al.⁵²52. Skuza G, Sadaj W, Kabziński M, Cassano G, Gasparre G, Abate C, et al. The effects of new sigma (σ) receptor ligands, PB190 and PB212, in the models predictive of antidepressant activity. Pharmacol Rep. 2014;66:320-4.	Mouse (male)	(10)	Acute (i.p.)	+ σ₁ receptor agonist PB190	FSTTST	FST: ↓ immobility time TST: no effect Locomotor activity: NE	σ₁ receptor agonist had no effect on antidepressant-like effects of amantadine

Reference	Disorder	Design	n	Evaluation scale	Amantadine dose (mg/day)	Treatment duration (weeks)	Result	Comments
Antidepressant studies
Vale et al.⁷¹71. Vale S, Espejel MA, Dominguez JC. Amantadine in depression. Lancet. 1971;2:437.	Chronic depressive syndrome	DB, R, C (placebo)	16-18/group	Zung SRS	100-200	4	67% of patients improved (vs. 25% in placebo group)	Diagnostic criteria not used Response: score below median
Stryjer et al.⁷²72. Stryjer R, Strous RD, Shaked G, Bar F, Feldman B, Kotler M, et al. Amantadine as augmentation therapy in the management of treatment-resistant depression. Int Clin Psychopharmacol. 2003;18:93-6.	MD (refractory)	Open Add-on	8	HDRS CGI	100-300	4	50% of patients responded (≥ 50% reduction)	Pre vs. post comparison
Antidepressant potentiation studies
Rogóz et al.⁵⁸58. Rogóz Z, Skuza G, Daniel WA, Wojcikowski J, Dudek D, Wrobel A. Amantadine as an additive treatment in patients suffering from drug-resistant unipolar depression. Pharmacol Rep. 2007;59:778-84.	MD (refractory)	Open + imipramine	25/group	HDRS	100	6	Potentiated effect of imipramine	Comparison between imipramine and imipramine + amantadine
Comorbidity/secondary depression
Ferszt et al.⁷³73. Ziedonis DM, Kosten TR. Pharmacotherapy improves treatment outcome in depressed cocaine addicts. J Psychoactive Drugs. 1991;23:417-25.	MD, bipolar depression, dysthymia + BDV infection	Open Add-on	30	MADRS	200-350	8-12	63% of patients improved (≥ 40% reduction)	Better response associated with Ag2 BDV antigen
Dietrich et al.⁷⁴74. Ferszt R, Kühl KP, Bode L, Severus EW, Winzer B, Berghöfer A, et al. Amantadine revisited: an open trial of amantadinesulfate treatment in chronically depressed patients with Borna disease virus infection. Pharmacopsychiatry. 1999;32:142-7.	MD, bipolar depression + BDV infection	Open Add-on	25	HDRS OCPCRIT	100-300	11 (mean)	68% of patients improved (≥ 50% reduction or two steps on OCPCRIT)
Ziedonis & Kosten⁷⁵75. Kronenberger B, Berg T, Herrmann E, Hinrichsen H, Gerlach T, Buggisch P, et al. Efficacy of amantadine on quality of life in patients with chronic hepatitis C treated with interferon-α and ribavirin: results from a randomized, placebo-controlled, double-blind trial. Eur J Gastroenterol Hepatol. 2007;19:639-46.	Depression secondary to cocaine addiction	DB, R, C (placebo/ desipramine)	5-9/group	BDI	300	12	Prevented increase in depression score	Reduced cocaine craving and consumption
Quarentini et al.⁷⁶76. Rogóz Z, Dziedzicka-Wasylewska M, Daniel WA, Wójcikowski J, Dudek D, Wróbel A, et al. Effects of joint administration of imipramine and amantadine in patients with drug-resistant unipolar depression. Pol J Pharmacol. 2004;56:735-42.	Depression induced by interferon-α	Single-blind add-on	6-8/group	HADS	200	24	Prevented depression	Exclusion criteria: history of depression
Kronenberger et al.⁷⁷77. Quarantini LC, Miranda-Scippa A, Schinoni MI, Sampaio AS, Santos-Jesus R, Bressan RA, et al. Effect of amantadine on depressive symptoms in chronic hepatitis C patients treated with pegylated interferon: a randomized, controlled pilot study. Clin Neuropharmacol. 2006;29:138-43.	Depression induced by interferon-α	DB, R, C (placebo)	131-136/group	POMS	200	48	No effect on POMS depression factor	Prevented depressive symptoms in a subset of patients

[1] Correspondence: Roberto Andreatini, Laboratório de Fisiologia e Farmacologia do Sistema Nervoso Central, Departamento de Farmacologia, Universidade Federal do Paraná, Centro Politécnico, Jardim das Américas, CEP 81540-990, Caixa Postal 19031, Curitiba, PR, Brazil. E-mail: randreatini@ufpr.br

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Potential antidepressant effect of amantadine: a review of preclinical studies and clinical trials

Objective:

Methods:

Results:

Conclusion: