Exploring multitarget interactions to reduce opiate withdrawal syndrome and psychiatric comorbidity

Fabio Del Bello; Eleonora Diamanti; Mario Giannella; Valerio Mammoli; Laura Mattioli; Federica Titomanlio; Alessandro Piergentili; Wilma Quaglia; Marco Lanza; Chiara Sabatini; Gianfranco Caselli; Elena Poggesi; Maria Pigini

doi:10.1021/ml400232p

Exploring multitarget interactions to reduce opiate withdrawal syndrome and psychiatric comorbidity

ACS Med Chem Lett. 2013 Jul 22;4(9):875-9. doi: 10.1021/ml400232p. eCollection 2013 Sep 12.

Affiliations

¹ School of Pharmacy, Medicinal Chemistry Unit, University of Camerino , Via S. Agostino 1, 62032 Camerino, Italy.
² School of Pharmacy, Pharmacognosy Unit, University of Camerino , Via Madonna delle Carceri 9, 62032 Camerino, Italy.
³ Pharmacology & Toxicology Department, Rottapharm-Madaus , 20052 Monza, Italy.
⁴ Recordati S.pA., Drug Discovery , Via Civitali 1, 20148 Milano, Italy.

Abstract

Opioid addiction is often characterized as a chronic relapsing condition due to the severe somatic and behavioral signs, associated with depressive disorders, triggered by opiate withdrawal. Since prolonged abstinence remains a major challenge, our interest has been addressed to such objective. Exploring multitarget interactions, the present investigation suggests that 3 or its (S)-enantiomer and 4, endowed with effective α2C-AR agonism/α2A-AR antagonism/5-HT1A-R agonism, or 7 and 9-11 producing efficacious α2C-AR agonism/α2A-AR antagonism/I2-IBS interaction might represent novel multifunctional tools potentially useful for reducing withdrawal syndrome and associated depression. Such agents, lacking in sedative side effects due to their α2A-AR antagonism, might afford an improvement over current therapies with clonidine-like drugs.

Keywords: 5-HT1A agonists; I2−IBS ligands; antidepressant-like effect; morphine withdrawal symptoms reduction; α2-Adrenergic ligands.