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Obsessive-compulsive disorder, impulse control disorders and drug addiction: common features and potential treatments.

机译:强迫症,冲动控制障碍和药物成瘾:共同特征和潜在治疗方法。

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摘要

The basic concepts underlying compulsive, impulsive and addictive behaviours overlap, which may help explain why laymen use these expressions interchangeably. Although there has been a large research effort to better characterize and disentangle these behaviours, clinicians and scientists are still unable to clearly differentiate them. Accordingly, obsessive-compulsive disorder (OCD), impulse control disorders (ICD) and substance-related disorders (SUD) overlap on different levels, including phenomenology, co-morbidity, neurocircuitry, neurocognition, neurochemistry and family history. In this review we summarize these issues with particular emphasis on the role of the opioid system in the pathophysiology and treatment of OCD, ICD and SUD. We postulate that with progression and chronicity of OCD, the proportion of the OCD-related behaviours (e.g. checking, washing, ordering and hoarding, among others) that are driven by impulsive 'rash' processes increase as involvement of more ventral striatal circuits becomes prominent. In contrast, as SUD and ICD progress, the proportion of the SUD- and ICD-related behaviours that are driven by compulsive 'habitual' processes increase as involvement of more dorsal striatal circuits become prominent. We are not arguing that, with time, ICD becomes OCD or vice versa. Instead, we are proposing that these disorders may acquire qualities of the other with time. In other words, while patients with ICD/SUD may develop 'compulsive impulsions', patients with OCD may exhibit 'impulsive compulsions'. There are many potential implications of our model. Theoretically, OCD patients exhibiting impulsive or addictive features could be managed with drugs that address the quality of the underlying drives and the involvement of neural systems. For example, agents for the reduction or prevention of relapse of addiction (e.g. heavy drinking), which modulate the cortico-mesolimbic dopamine system through the opioid (e.g. buprenorphine and naltrexone), glutamate (e.g. topiramate), serotonin (e.g. ondansetron) or gamma-aminobutyric acid (e.g. baclofen and topiramate) systems, may prove to show some benefit in certain forms of OCD. Based on the available evidence, we suggest that the treatment of patients with these disorders must account for alterations in the underlying motivations and neurobiology of the condition. We provide an initial guide to the specific treatments that future clinical trials might consider in patients with OCD. For example, it might be wise to test naltrexone in patients with co-morbid SUD and ICD, topiramate in patients with co-morbid ICD and eating disorders, and baclofen in patients with co-morbid Tourette's syndrome. These trials could also include scales aimed at assessing underlying impulsivity (e.g. Barratt Impulsiveness Scale) to check whether this construct might predict response to drugs acting on the reward system.
机译:强迫,冲动和上瘾行为的基本概念重叠,这可能有助于解释为什么外行人可以交替使用这些表达方式。尽管已经进行了大量的研究来更好地表征和区分这些行为,但是临床医生和科学家仍然无法清楚地区分这些行为。因此,强迫症(OCD),冲动控制障碍(ICD)和与物质有关的障碍(SUD)在不同的水平上重叠,包括现象学,合并症,神经回路,神经认知,神经化学和家族史。在这篇综述中,我们总结了这些问题,并特别强调了阿片类药物系统在强迫症,强迫症和超氧化物歧化酶的病理生理和治疗中的作用。我们假设随着强迫症的进展和慢性,由冲动性“皮疹”过程驱动的强迫症相关行为(例如检查,洗涤,整理和ho积等)的比例随着更多腹侧纹状体回路的介入而增加。相反,随着SUD和ICD的发展,强迫性“习惯”过程驱动的SUD和ICD相关行为的比例随着更多背侧纹状体回路的介入而增加。我们并不是说随着时间的流逝,ICD会变成OCD,反之亦然。相反,我们建议这些疾病可能会随着时间的推移获得其他疾病的特质。换句话说,尽管ICD / SUD患者可能会出现“强迫性冲动”,而OCD患者可能会表现出“冲动性冲动”。我们的模型有许多潜在的含义。从理论上讲,具有冲动或上瘾特征的强迫症患者可以用能解决潜在的驱动器质量和神经系统受累的药物进行治疗。例如,用于减少或预防成瘾复发(例如大量饮酒)的药物,它们通过阿片类药物(例如丁丙诺啡和纳曲酮),谷氨酸盐(例如托吡酯),5-羟色胺(例如恩丹西酮)或γ调节皮质-中脑多巴胺系统-氨基丁酸(例如巴氯芬和托吡酯)系统可能会在某些形式的强迫症中显示出某些益处。根据现有证据,我们建议对这些疾病的患者进行治疗必须考虑该病的潜在动机和神经生物学改变。我们为将来的临床试验可能考虑在强迫症患者中使用的特定治疗方法提供了初步指南。例如,在患有合并症的SUD和ICD患者中测试纳曲酮,在合并症的ICD和进食障碍患者中测试托吡酯,在合并症的Tourette综合征患者中测试巴氯芬可能是明智的。这些试验还可以包括旨在评估潜在冲动的量表(例如Barratt冲动量表),以检查该结构是否可以预测对作用于奖励系统的药物的反应。

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