Cocaine self-administration behavior is associated with subcortical and cortical morphometry measures in individuals with cocaine use disorder.

IF 2.7 3区 医学 Q2 PSYCHOLOGY, CLINICAL American Journal of Drug and Alcohol Abuse Pub Date : 2024-05-03 Epub Date: 2024-03-29 DOI:10.1080/00952990.2024.2318585
Robert J Kohler, Simon Zhornitsky, Marc N Potenza, Sarah W Yip, Patrick Worhunsky, Gustavo A Angarita
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Abstract

Background: Individual differences in gray-matter morphometry in the limbic system and frontal cortex have been linked to clinical features of cocaine use disorder (CUD). Self-administration paradigms can provide more direct measurements of the relationship between the regulation of cocaine use and gray-matter morphometry when compared to self-report assessments.Objectives: Our goal was to investigate associations with self-administration behavior in subcortical and cortical brain regions. We hypothesized the number of cocaine infusions self-administered would be correlated with gray-matter volumes (GMVs) in the striatum, amygdala, and hippocampus. Due to scarcity in human studies, we did not hypothesize subcortical directionality. In the frontal cortex, we hypothesized thickness would be negatively correlated with self-administered cocaine.Methods: We conducted an analysis of cocaine self-administration and structural MRI data from 33 (nFemales = 10) individuals with moderate-to-severe CUD. Self-administration lasted 60-minutes and cocaine (8, 16, or 32 mg/70 kg) was delivered on an FR1 schedule (5-minute lockout). Subcortical and cortical regression analyses were performed that included combined bilateral regions and age, experimental variables and use history as confounders.Results: Self-administered cocaine infusions were positively associated with caudal GMV (b = 0.18, p = 0.030) and negatively with putamenal GMV (b = -0.10, p = 0.041). In the cortical model, infusions were positively associated with insular thickness (b = 0.39, p = 0.008) and women appeared to self-administer cocaine more frequently (b = 0.23, p = 0.019).Conclusions: Brain morphometry features in the striatum and insula may contribute to cocaine consumption in CUD. These differences in morphometry may reflect consequences of prolonged use, predisposed vulnerability, or other possibilities.Clinical Trial Numbers: NCT01978431; NCT03471182.

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可卡因使用障碍患者的可卡因自我给药行为与皮层下和皮层形态测量相关。
背景:边缘系统和额叶皮层灰质形态的个体差异与可卡因使用障碍(CUD)的临床特征有关。与自我报告评估相比,自我给药范式可以更直接地测量可卡因使用调节与灰质形态测量之间的关系:我们的目标是研究皮质下和皮质脑区与自我给药行为之间的关联。我们假设自我注射可卡因的次数与纹状体、杏仁核和海马的灰质体积(GMVs)相关。由于缺乏人体研究,我们没有假设皮层下的方向性。在额叶皮层,我们假设其厚度与自我吸食可卡因呈负相关:我们对 33 名中度至重度 CUD 患者(女性 = 10 人)的可卡因自我给药和结构性 MRI 数据进行了分析。自我给药持续 60 分钟,可卡因(8、16 或 32 毫克/70 千克)按 FR1 计划给药(5 分钟锁定)。研究人员对皮层下和皮层进行了回归分析,将双侧区域以及年龄、实验变量和使用史作为混杂因素进行了综合分析:结果:自控可卡因输注与尾状GMV呈正相关(b = 0.18,p = 0.030),与正视图GMV呈负相关(b = -0.10,p = 0.041)。在皮层模型中,输注与岛叶厚度呈正相关(b = 0.39,p = 0.008),女性似乎更频繁地自我注射可卡因(b = 0.23,p = 0.019):结论:纹状体和岛叶的大脑形态特征可能会导致 CUD 的可卡因消费。这些形态学上的差异可能反映了长期使用的后果、易感性或其他可能性:NCT01978431;NCT03471182。
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来源期刊
CiteScore
4.70
自引率
3.70%
发文量
68
期刊介绍: The American Journal of Drug and Alcohol Abuse (AJDAA) is an international journal published six times per year and provides an important and stimulating venue for the exchange of ideas between the researchers working in diverse areas, including public policy, epidemiology, neurobiology, and the treatment of addictive disorders. AJDAA includes a wide range of translational research, covering preclinical and clinical aspects of the field. AJDAA covers these topics with focused data presentations and authoritative reviews of timely developments in our field. Manuscripts exploring addictions other than substance use disorders are encouraged. Reviews and Perspectives of emerging fields are given priority consideration. Areas of particular interest include: public health policy; novel research methodologies; human and animal pharmacology; human translational studies, including neuroimaging; pharmacological and behavioral treatments; new modalities of care; molecular and family genetic studies; medicinal use of substances traditionally considered substances of abuse.
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