Prazosin and cyproheptadine in combination in the treatment of alcohol use disorder: A randomized, double‐blind, placebo‐controlled trial-Reference-Cited by-同舟云学术

Prazosin and cyproheptadine in combination in the treatment of alcohol use disorder: A randomized, double‐blind, placebo‐controlled trial

Published:2024-04-10 Issue:7 Volume:119 Page:1211-1223
ISSN:0965-2140
Container-title:Addiction
language:en
Short-container-title:Addiction

Author:

Aubin Henri‐Jean¹^ORCID,Berlin Ivan²^ORCID,Guiraud Julien³⁴,Bruhwyler Jacques⁵,Batel Philippe⁶,Perney Pascal⁷,Trojak Benoît⁸,Bendimerad Patrick⁹,Guillou Morgane¹⁰^ORCID,Bisch Michaël¹¹,Grall‐Bronnec Marie¹²^ORCID,Labarrière Damien¹³,Delsart Dominique¹⁴,Questel Frank¹⁵,Moirand Romain¹⁶,Bernard Philippe¹⁷,Trovero Fabrice¹⁸,Pham Hang Phuong¹⁹,Tassin Jean‐Pol²⁰,Puech Alain¹⁷²⁰

Affiliation:

1. Université Paris‐Saclay, AP‐HP, Inserm, CESP Villejuif France

2. Hopital Pitie‐Salpetriere, Sorbonne Université Paris France

3. University of Amsterdam Amsterdam the Netherlands

4. Vergio Clichy France

5. ECSOR sa/nv Brussels Belgium

6. Centre Hospitalier Camille Claudel La Couronne France

7. Hôpital Carémeau, Nîmes, Université Montpellier 1 Villejuif France

8. Centre hospitalier Universitaire Dijon Bourgogne, Université Bourgogne Franche‐Comté Besançon France

9. Addiction Department, Groupe Hospitalier Littoral Atlantique La Rochelle France

10. ER 7479 SPURBO, Université Bretagne Occidentale Brest France

11. Centre Psychothérapique de Nancy, Addiction Medicine department Laxou France

12. Addictology and Liaison Psychiatry Department, Nantes University Hospital, Nantes and Tours Universities Nantes France

13. Centre Hospitalier Régional Orléans France

14. Private practice Bersée France

15. Université Paris Diderot, GH Lariboisière‐Saint‐Louis‐Fernand Widal Paris France

16. Université Rennes, Rennes, Institut NUMECAN (Nutrition Metabolisms and Cancer), UF Addictologie Rennes France

17. Kinnov‐Therapeutics Orléans France

18. SAS Key‐Obs Orléans France

19. Parean Biotechnologies Saint‐Malo France

20. Inserm, Sorbonne‐Université, Laboratoire Neuroscience Paris‐Seine Paris France

Abstract

AbstractBackground and aimsPre‐clinical studies suggest that the simultaneous blockade of the α1b and 5HT2A receptors may be effective in reducing alcohol consumption. This study aimed to assess the efficacy and safety of prazosin (α1b blocker) and cyproheptadine (5HT2A blocker) combination in decreasing total alcohol consumption (TAC) in alcohol use disorder (AUD).Design, setting and participantsThis was a double‐blind, parallel group, placebo‐controlled, Phase 2, randomized clinical trial conducted in 32 addiction treatment centres in France. A total of 108 men and 46 women with severe AUD took part.InterventionParticipants were randomly assigned to one of the following 3‐month treatments: (1) low‐dose group (LDG) receiving 8 mg cyproheptadine and 5 mg prazosin extended‐release (ER) formulation daily; (2) high‐dose group (HDG) receiving 12 mg cyproheptadine and 10 mg prazosin ER daily; and (3) placebo group (PG) receiving placebo of cyproheptadine and prazosin ER. A total of 154 patients were randomized: 54 in the PG, 54 in the LDG and 46 in the HDG.MeasurementsThe primary outcome was TAC change from baseline to month 3.FindingsA significant main treatment effect in the change in TAC was found in the intent‐to‐treat population (P = 0.039). The HDG and LDG showed a benefit in the change in TAC from baseline to month 3 compared with PG: −23.6 g/day, P = 0.016, Cohen's d = −0.44; −18.4 g/day, P = 0.048 (Bonferroni correction P < 0.025), Cohen's d = −0.36. In a subgroup of very high‐risk drinking‐level participants (> 100 g/day of pure alcohol for men and > 60 g/day for women), the difference between the HDG and the PG in the primary outcome was −29.8 g/day (P = 0.031, Cohen's d = −0.51). The high and low doses were well‐tolerated with a similar safety profile.ConclusionsA randomized controlled trial of treatment of severe alcohol use disorder with a cyproheptadine−prazosin combination for 3 months reduced drinking by more than 23 g per day compared with placebo. A higher dose combination was associated with a larger magnitude of drinking reduction than a lower dose combination while showing similar safety profile.

Funder

Horizon 2020 Framework Programme

Biocodex Microbiota Foundation

Bpifrance

Publisher

Wiley

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1111/add.16484

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