Pharmacology and Therapeutic Potential of Benzothiazole Analogues for Cocaine Use Disorder

Abstract: Pharmacological targeting of the dopamine D 4 receptor (D 4 R)� expressed in brain regions that control cognition, attention, and decision-making�could be useful for several neuropsychiatric disorders including substance use disorders (SUDs). This study focused on the synthesis and evaluation of a novel series of benzothiazole analogues designed to target D 4 R. We identified several compounds with high D 4 R binding affinity (K i ≤ 6.9 nM) and >91-fold selectivity over other D 2 -like receptors (D 2 R, D 3 R)… Show more

“…For instance, antagonism or partial agonism of D 2 R has been demonstrated to worsen Parkinsonism, while action at D 1 R in conjunction with levodopa administration is associated with increased LID severity. − Therefore, the pursuit of D 4 R antagonists for PD therapy demands meticulous attention to the selectivity and efficacy of the designed compounds. Recent advances in synthetic chemistry, structural biology, and pharmacology have enabled the design and characterization of diverse selective D 4 R antagonists, as exemplified in several key studies. ,− Building off of these rich structure–activity relationship data, we disclose herein the development of a novel class of potent, selective D 4 R antagonists suitable for further preclinical optimization.…”

Computer-Aided Design and Biological Evaluation of Diazaspirocyclic D₄R Antagonists

“…For instance, antagonism or partial agonism of D 2 R has been demonstrated to worsen Parkinsonism, while action at D 1 R in conjunction with levodopa administration is associated with increased LID severity. − Therefore, the pursuit of D 4 R antagonists for PD therapy demands meticulous attention to the selectivity and efficacy of the designed compounds. Recent advances in synthetic chemistry, structural biology, and pharmacology have enabled the design and characterization of diverse selective D 4 R antagonists, as exemplified in several key studies. ,− Building off of these rich structure–activity relationship data, we disclose herein the development of a novel class of potent, selective D 4 R antagonists suitable for further preclinical optimization.…”

Computer-Aided Design and Biological Evaluation of Diazaspirocyclic D₄R Antagonists