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Dopamine dysregulation syndrome: an overview of its epidemiology, mechanisms and management.

机译:多巴胺失调综合症:其流行病学,机制和治疗的概述。

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Dopamine dysregulation syndrome (DDS) is a relatively recently described iatrogenic disturbance that may complicate long-term symptomatic therapy of Parkinson's disease. Patients with DDS develop an addictive pattern of dopamine replacement therapy (DRT) use, administering doses in excess of those required to control their motor symptoms. The prevalence of DDS in patients attending specialist Parkinson's disease centres is 3-4%. Amongst the behavioural disturbances associated with DDS are punding, which is a complex stereotyped behaviour, and impulse control disorders (ICDs), such as pathological gambling, hypersexuality, compulsive shopping and compulsive eating. We review the risk factors and potential mechanisms for the development of DDS, including personality traits, potential genetic influences and Parkinson's disease-related cognitive deficits. Impulsive personality traits are prominent in patients developing DDS, and have been previously associated with the development of substance dependence. Candidate genes affecting the dopamine 'D(2)-like' receptor family have been associated with impulsive personality traits in addition to drug and nondrug addictions. Impaired decision making is implicated in addictive behaviours, and decision-making abilities can be influenced by dopaminergic medications. In Parkinson's disease, disruption of the reciprocal loops between the striatum and structures in the prefrontal cortex following dopamine depletion may predispose to DDS. The role of DRT in DDS is discussed, with particular reference to models of addiction, suggesting that compulsive drug use is due to progressive neuroadaptations in dopamine projections to the accumbens-related circuitry. Evidence for neuroadaptations and sensitization occurring in DDS include enhanced levodopa-induced ventral striatal dopamine release. Levodopa is still considered the most potent trigger for DDS in Parkinson's disease, but subcutaneous apomorphine and oral dopamine agonists may also be responsible. In the management of DDS, further research is needed to identify at-risk groups, thereby facilitating more effective early intervention. Therefore, an increased awareness of the syndrome amongst treating physicians is vital. Medication reduction strategies are employed, particularly with regard to avoiding rapidly acting 'booster' DRT formulations. Psychosocial treatments, including cognitive-behavioural therapy, have been beneficial in treating substance use disorders and ICDs in non-Parkinson's disease patients, but there are currently no published trials of psychological interventions in DDS. Further studies are also required to identify factors that can predict those patients with DDS or ICDs who will derive benefit from surgical interventions such as deep brain stimulation.
机译:多巴胺失调综合症(DDS)是一种相对较新近描述的医源性疾病,可能会使帕金森氏病的长期对症治疗复杂化。 DDS患者会产生使用多巴胺替代疗法(DRT)的成瘾模式,其给药剂量应超过控制其运动症状所需的剂量。在帕金森专科疾病中心就诊的患者中DDS的患病率为3-4%。与DDS相关的行为障碍包括打p,这是一种复杂的定型行为,以及冲动控制障碍(ICD),例如病理性赌博,性欲亢进,强迫性购物和强迫性进食。我们审查了发展DDS的危险因素和潜在机制,包括人格特质,潜在的遗传影响和帕金森氏病相关的认知缺陷。冲动型人格特征在发展DDS的患者中很突出,并且以前与物质依赖的发展有关。影响多巴胺“ D(2)样”受体家族的候选基因除药物和非药物成瘾外,还与冲动型人格特征相关。上瘾的行为可能会影响决策能力,多巴胺能药物会影响决策能力。在帕金森氏病中,多巴胺耗竭后纹状体与前额叶皮层结构之间的相互循环中断可能是DDS的诱因。讨论了DRT在DDS中的作用,并特别参考了成瘾模型,这表明强迫性药物的使用是由于多巴胺投射到伏安相关系统的过程中进行性神经适应。 DDS中发生神经适应和敏化的证据包括左旋多巴诱导的腹侧纹状体多巴胺释放增强。左旋多巴仍被认为是帕金森氏病中DDS的最有效诱因,但皮下的阿扑吗啡和口服多巴胺激动剂也可能是造成这种情况的原因。在DDS的管理中,需要进一步的研究来确定高危人群,从而促进更有效的早期干预。因此,在治疗医师中提高对该综合征的认识是至关重要的。采用药物减少策略,尤其是在避免快速起效的“助推器” DRT制剂方面。心理社会疗法,包括认知行为疗法,对于治疗非帕金森氏病患者的药物滥用和ICD有益,但目前尚无关于DDS心理干预的公开试验。还需要进一步的研究来确定可以预测那些DDS或ICD患者将从外科手术干预(例如深部脑刺激)中获益的因素。

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