Antiviral treatment perspective against Borna disease virus 1 infection in major depression: a double-blind placebo-controlled randomized clinical trial.
Adult
Amantadine
/ pharmacology
Animals
Antibodies, Viral
/ blood
Antidepressive Agents
/ pharmacology
Antigens, Viral
/ blood
Antiviral Agents
/ pharmacology
Bipolar Disorder
/ drug therapy
Borna Disease
/ drug therapy
Borna disease virus
/ drug effects
Cells, Cultured
Cross-Over Studies
Depressive Disorder, Major
/ drug therapy
Double-Blind Method
Female
Humans
Male
Middle Aged
Rabbits
Virus Replication
/ drug effects
Borna disease virus 1 (BDV-1)
Major depression
amantadine
antiviral treatment
bipolar disorder
double-blind placebo-controlled randomized clinical trial (RCT)
Journal
BMC pharmacology & toxicology
ISSN: 2050-6511
Titre abrégé: BMC Pharmacol Toxicol
Pays: England
ID NLM: 101590449
Informations de publication
Date de publication:
17 02 2020
17 02 2020
Historique:
received:
29
03
2019
accepted:
05
02
2020
entrez:
19
2
2020
pubmed:
19
2
2020
medline:
5
11
2020
Statut:
epublish
Résumé
Whether Borna disease virus (BDV-1) is a human pathogen remained controversial until recent encephalitis cases showed BDV-1 infection could even be deadly. This called to mind previous evidence for an infectious contribution of BDV-1 to mental disorders. Pilot open trials suggested that BDV-1 infected depressed patients benefitted from antiviral therapy with a licensed drug (amantadine) which also tested sensitive in vitro. Here, we designed a double-blind placebo-controlled randomized clinical trial (RCT) which cross-linked depression and BDV-1 infection, addressing both the antidepressant and antiviral efficacy of amantadine. The interventional phase II RCT (two 7-weeks-treatment periods and a 12-months follow-up) at the Hannover Medical School (MHH), Germany, assigned currently depressed BDV-1 infected patients with either major depression (MD; N = 23) or bipolar disorder (BD; N = 13) to amantadine sulphate (PK-Merz®; twice 100 mg orally daily) or placebo treatment, and contrariwise, respectively. Clinical changes were assessed every 2-3 weeks by the 21-item Hamilton rating scale for depression (HAMD) (total, single, and combined scores). BDV-1 activity was determined accordingly in blood plasma by enzyme immune assays for antigens (PAG), antibodies (AB) and circulating immune complexes (CIC). Primary outcomes (≥25% HAMD reduction, week 7) were 81.3% amantadine vs. 35.3% placebo responder (p = 0.003), a large clinical effect size (ES; Cohen's d) of 1.046, and excellent drug tolerance. Amantadine was safe reducing suicidal behaviour in the first 2 weeks. Pre-treatment maximum infection levels were predictive of clinical improvement (AB, p = 0.001; PAG, p = 0.026; HAMD week 7). Respective PAG and CIC levels correlated with AB reduction (p = 0,001 and p = 0.034, respectively). Follow-up benefits (12 months) correlated with dropped cumulative infection measures over time (p < 0.001). In vitro, amantadine concentrations as low as 2.4-10 ng/mL (50% infection-inhibitory dose) prevented infection with human BDV Hu-H1, while closely related memantine failed up to 100,000-fold higher concentration (200 μg/mL). Our findings indicate profound antidepressant efficacy of safe oral amantadine treatment, paralleling antiviral effects at various infection levels. This not only supports the paradigm of a link of BDV-1 infection and depression. It provides a novel possibly practice-changing low cost mental health care perspective for depressed BDV-1-infected patients addressing global needs. The trial was retrospectively registered in the German Clinical Trials Registry on 04th of March 2015. The trial ID is DRKS00007649; https://www.drks.de/drks_web/setLocale_EN.do.
Sections du résumé
BACKGROUND
Whether Borna disease virus (BDV-1) is a human pathogen remained controversial until recent encephalitis cases showed BDV-1 infection could even be deadly. This called to mind previous evidence for an infectious contribution of BDV-1 to mental disorders. Pilot open trials suggested that BDV-1 infected depressed patients benefitted from antiviral therapy with a licensed drug (amantadine) which also tested sensitive in vitro. Here, we designed a double-blind placebo-controlled randomized clinical trial (RCT) which cross-linked depression and BDV-1 infection, addressing both the antidepressant and antiviral efficacy of amantadine.
METHODS
The interventional phase II RCT (two 7-weeks-treatment periods and a 12-months follow-up) at the Hannover Medical School (MHH), Germany, assigned currently depressed BDV-1 infected patients with either major depression (MD; N = 23) or bipolar disorder (BD; N = 13) to amantadine sulphate (PK-Merz®; twice 100 mg orally daily) or placebo treatment, and contrariwise, respectively. Clinical changes were assessed every 2-3 weeks by the 21-item Hamilton rating scale for depression (HAMD) (total, single, and combined scores). BDV-1 activity was determined accordingly in blood plasma by enzyme immune assays for antigens (PAG), antibodies (AB) and circulating immune complexes (CIC).
RESULTS
Primary outcomes (≥25% HAMD reduction, week 7) were 81.3% amantadine vs. 35.3% placebo responder (p = 0.003), a large clinical effect size (ES; Cohen's d) of 1.046, and excellent drug tolerance. Amantadine was safe reducing suicidal behaviour in the first 2 weeks. Pre-treatment maximum infection levels were predictive of clinical improvement (AB, p = 0.001; PAG, p = 0.026; HAMD week 7). Respective PAG and CIC levels correlated with AB reduction (p = 0,001 and p = 0.034, respectively). Follow-up benefits (12 months) correlated with dropped cumulative infection measures over time (p < 0.001). In vitro, amantadine concentrations as low as 2.4-10 ng/mL (50% infection-inhibitory dose) prevented infection with human BDV Hu-H1, while closely related memantine failed up to 100,000-fold higher concentration (200 μg/mL).
CONCLUSIONS
Our findings indicate profound antidepressant efficacy of safe oral amantadine treatment, paralleling antiviral effects at various infection levels. This not only supports the paradigm of a link of BDV-1 infection and depression. It provides a novel possibly practice-changing low cost mental health care perspective for depressed BDV-1-infected patients addressing global needs.
TRIAL REGISTRATION
The trial was retrospectively registered in the German Clinical Trials Registry on 04th of March 2015. The trial ID is DRKS00007649; https://www.drks.de/drks_web/setLocale_EN.do.
Identifiants
pubmed: 32066504
doi: 10.1186/s40360-020-0391-x
pii: 10.1186/s40360-020-0391-x
pmc: PMC7027224
doi:
Substances chimiques
Antibodies, Viral
0
Antidepressive Agents
0
Antigens, Viral
0
Antiviral Agents
0
Amantadine
BF4C9Z1J53
Banques de données
DRKS
['DRKS00007649']
Types de publication
Clinical Trial, Phase II
Journal Article
Randomized Controlled Trial
Langues
eng
Sous-ensembles de citation
IM
Pagination
12Références
J Virol. 1994 Mar;68(3):1382-96
pubmed: 7906311
Bipolar Disord. 2000 Mar;2(1):65-70
pubmed: 11254023
PLoS Pathog. 2010 Jul 29;6(7):e1001030
pubmed: 20686665
Lancet. 1997 Jun 21;349(9068):1813-4
pubmed: 9269221
N Engl J Med. 2018 Oct 4;379(14):1375-1377
pubmed: 30281979
Proc Natl Acad Sci U S A. 1994 May 10;91(10):4362-6
pubmed: 8183914
N Engl J Med. 2014 Feb 6;370(6):498-501
pubmed: 24428425
N Engl J Med. 2018 Oct 4;379(14):1377-1379
pubmed: 30281984
APMIS Suppl. 2008;(124):53-7
pubmed: 18771099
Eur J Neurol. 2009 Mar;16(3):399-403
pubmed: 19364367
J Affect Disord. 2006 Jan;90(1):43-7
pubmed: 16324750
Ther Adv Psychopharmacol. 2012 Oct;2(5):179-88
pubmed: 23983973
J Affect Disord. 2014 Mar;156:24-35
pubmed: 24388038
N Engl J Med. 2008 Jan 17;358(3):252-60
pubmed: 18199864
APMIS Suppl. 2008;(124):61-5
pubmed: 18771101
Science. 1985 May 10;228(4700):755-6
pubmed: 3922055
Med Sci Monit. 2002 Sep;8(9):CR642-6
pubmed: 12218946
PLoS One. 2014 Apr 02;9(4):e91936
pubmed: 24694747
Virology. 1996 Sep 15;223(2):272-82
pubmed: 8806563
Pharmacopsychiatry. 1999 Jul;32(4):142-7
pubmed: 10505484
Pharmacopsychiatry. 1999 Mar;32(2):47-55
pubmed: 10333162
Lancet. 1997 Jan 18;349(9046):178-9
pubmed: 9111548
Am J Psychiatry. 2006 Jan;163(1):153-5
pubmed: 16390905
Nat Med. 1995 Mar;1(3):232-6
pubmed: 7585039
BMJ. 2008 Mar 8;336(7643):516-7
pubmed: 18319297
Mol Psychiatry. 2012 May;17(5):486-93
pubmed: 22290118
BMC Med. 2016 Jan 22;14:9
pubmed: 26801406
Transl Psychiatry. 2016 Jun 07;6(6):e834
pubmed: 27271860
BMC Psychiatry. 2010 Sep 08;10:70
pubmed: 20825673
J Virol. 1996 Nov;70(11):7713-24
pubmed: 8892892
Arzneimittelforschung. 1970 Jul;20(7):915-8
pubmed: 5536059
Virol J. 2015 Mar 12;12:39
pubmed: 25888756
Clin Microbiol Rev. 2003 Jul;16(3):534-45
pubmed: 12857781
Br J Soc Clin Psychol. 1967 Dec;6(4):278-96
pubmed: 6080235
BMC Psychiatry. 2016 Nov 3;16(1):369
pubmed: 27809822
Pharmacopsychiatry. 1998 May;31(3):77-82
pubmed: 9657234
Acta Psychiatr Scand. 1997 Dec;96(6):412-5
pubmed: 9421336
Biol Psychiatry. 1989 Dec;26(8):818-28
pubmed: 2511930
Psychiatry Res. 2003 Sep 30;120(2):201-6
pubmed: 14527651
JAMA. 2004 Jul 21;292(3):338-43
pubmed: 15265848
J Clin Psychiatry. 2013 Oct;74(10):966-73
pubmed: 24229746
Pharmacopsychiatry. 2008 Sep;41(5):202-3
pubmed: 18763224
Mol Psychiatry. 1999 Jan;4(1):33-8
pubmed: 10089006
J Virol. 2000 May;74(10):4601-11
pubmed: 10775596
Antiviral Res. 2017 Jul;143:237-245
pubmed: 28465146
Arch Virol. 2015 Feb;160(2):621-32
pubmed: 25449305
Virol J. 2014 Sep 03;11:161
pubmed: 25186971
N Engl J Med. 2015 Jul 9;373(2):154-62
pubmed: 26154788
Sci Rep. 2014 Mar 31;4:4530
pubmed: 24681753
PLoS One. 2013 Jun 21;8(6):e66623
pubmed: 23805250
APMIS Suppl. 2008;(124):74-6
pubmed: 18771104
Eur J Clin Microbiol Infect Dis. 2014 Apr;33(4):621-7
pubmed: 24170181
Rev Med Virol. 2007 May-Jun;17(3):181-203
pubmed: 17342788
APMIS Suppl. 2008;(124):89-93
pubmed: 18771108
Nature. 1999 Nov 18;402(6759):297-301
pubmed: 10580501
Prog Med Virol. 1988;35:107-51
pubmed: 3051132
Arch Virol Suppl. 1993;7:111-33
pubmed: 8219797
Arch Virol. 1997;142(10):2035-42
pubmed: 9413511
PLoS Med. 2018 Mar 27;15(3):e1002535
pubmed: 29584730
Int J Mol Sci. 2015 Aug 17;16(8):19347-68
pubmed: 26287181
Neuroscientist. 2014 Feb;20(1):29-43
pubmed: 23439589
Nature. 2010 Jan 7;463(7277):84-7
pubmed: 20054395
J Med Virol. 1992 Apr;36(4):309-15
pubmed: 1578223
Front Biosci. 2002 Feb 01;7:d470-95
pubmed: 11815287
APMIS Suppl. 2008;(124):21-39
pubmed: 18771094
Mol Psychiatry. 2001 Jul;6(4):481-91
pubmed: 11443538
Mol Psychiatry. 1996 Jul;1(3):200-12
pubmed: 9118344
J Virol. 1999 Sep;73(9):7903-6
pubmed: 10438889
Med Microbiol Immunol. 1998 Mar;186(4):195-200
pubmed: 9574902
PLoS Med. 2008 Feb;5(2):e45
pubmed: 18303940
Virus Res. 1996 Sep;44(1):33-44
pubmed: 8873411
Arch Virol. 1997;142(10):2043-8
pubmed: 9413512
J Clin Virol. 2006 Aug;36(4):309-11
pubmed: 16822717
PLoS One. 2013 Sep 09;8(9):e73973
pubmed: 24040131