Evaluation of the antidepressant therapeutic potential of isocyanine and pseudoisocyanine analogues of the organic cation decynium-22

2017 
Abstract Herein we describe the synthesis and evaluation of antidepressant properties of seven analogues ( 1–7 ) of the low affinity/high capacity transporter blocker decynium-22 (D-22). All analogues ( 1–7 ) were synthesized via base promoted coupling reactions between N -alkylated-2-methylquinolinium iodides or N -alkylated-4-methylquinolinium iodides and electrophilic N -alkylated-2-iodoquinolinium iodides. All final compounds were purified by re-crystallization or preparative HPLC and initial evaluation studies included; 1) screening for in vitro α1-adrenoceptor activity (a property that can lead to unwanted side-effects), 2) measuring antidepressant-like activity in a mouse tail suspension test (TST), and 3) measuring effects upon mouse locomotion. The results showed some analogues have lower affinities at α1-adrenoceptors compared to D-22 and showed antidepressant-like activity without the need for co-administration of SSRIs. Additionally, many analogues did not affect mouse locomotion to the same extent as D-22. Plans for additional evaluations of these promising analogues, including measurement of antidepressant-like activity with co-administration of selective serotonin re-uptake inhibitors (SSRIs), are outlined.
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