Tabernanthalog Reduces Motivation for Heroin and Alcohol in a Polydrug Use Model.

Psychedelic medicine (New Rochelle, N.Y.) Pub Date : 2023-06-01 Epub Date: 2023-06-14 DOI:10.1089/psymed.2023.0009
Jasper A Heinsbroek, Giuseppe Giannotti, Joel Bonilla, David E Olson, Jamie Peters
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Abstract

Background: The potential use of psychedelic drugs as therapeutics for neuropsychiatric disorders has been limited by their hallucinogenic properties. To overcome this limitation, we developed and characterized tabernanthalog (TBG), a novel analogue of the indole alkaloids ibogaine and 5-methoxy-N,N-dimethyltryptamine with reduced cardiac arrhythmogenic risk and a lack of classical psychedelic drugs-induced sensory alterations. We previously demonstrated that TBG has therapeutic efficacy in a preclinical model of opioid use disorder (OUD) in rats and in a binge model of alcohol drinking in mice. Alcohol is commonly co-used in ∼35-50% of individuals with OUD, and yet, preclinical models that recapitulate this comorbidity are lacking.

Methodology: Here we employed a polydrug model of heroin and alcohol couse to screen the therapeutic efficacy of TBG on metrics of both opioid and alcohol seeking. We first exposed rats to alcohol (or control sucrose-fade solution) in the home-cage (HC), using a two-bottle binge protocol, over a period of 1 month. Rats were then split into two groups that underwent self-administration training for either intravenous heroin or oral alcohol, so that we could assess the impact of HC alcohol exposure on the self-administration of each substance separately. Thereafter, rats began self-administering both heroin and alcohol in the same sessions. Finally, we tested the effects of TBG on break points for heroin and alcohol in a progressive ratio test, where the number of lever presses required to obtain a single reward increased exponentially.

Results and conclusion: TBG effectively reduced motivation for heroin and alcohol in this test, indicating its efficacy is preserved in animals with a history of heroin and alcohol polydrug use.

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在多药使用模型中,Tabernanthalog 可降低海洛因和酒精的使用动机。
背景:迷幻药的致幻特性限制了其作为神经精神疾病治疗药物的潜在用途。为了克服这一限制,我们开发并鉴定了 tabernanthalog (TBG),它是吲哚生物碱伊博格碱和 5-甲氧基-N,N-二甲基色胺的新型类似物,具有较低的致心律失常风险,并且没有传统迷幻药引起的感觉改变。我们以前曾证明,TBG 在大鼠阿片类药物使用障碍(OUD)的临床前模型和小鼠酗酒模型中具有疗效。方法:在此,我们采用海洛因和酒精的多药模型来筛选 TBG 对阿片类药物和酒精寻求指标的疗效。我们首先在家庭笼(HC)中采用两瓶狂饮方案让大鼠接触酒精(或蔗糖淡化溶液对照),为期 1 个月。然后,大鼠被分成两组,分别接受静脉注射海洛因或口服酒精的自我给药训练,这样我们就能分别评估HC酒精暴露对每种物质自我给药的影响。此后,大鼠开始在同一疗程中自我给药海洛因和酒精。最后,我们在渐进比率测试中测试了 TBG 对海洛因和酒精断点的影响,在该测试中,获得单次奖励所需的按压杠杆次数呈指数增长:结果和结论:在该测试中,TBG 能有效降低海洛因和酒精的刺激性,这表明它对有海洛因和酒精多种药物使用史的动物仍有疗效。
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