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Pharmacological Approaches to the Management of Binge Eating Disorder

机译:狂犬病患者的药理方法

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摘要

In the USA, binge eating disorder (BED) is the most common eating disorder, with a lifetime prevalence of similar to 3.5 % in adult women, 2.0 % in adult men, and 1.6 % in adolescents. BED is characterized by frequent episodes of binge eating that are accompanied by a sense of loss of control over eating and result in marked psychological distress. BED is highly co-morbid with obesity and with depression and other psychiatric conditions, and it is associated with substantial role impairment. Currently, there are no US FDA-approved pharmacological treatments for BED. Animal and human studies implicate underlying dysregulation in dopamine, opioid, acetylcholine, and serotonin neurocircuitry within brain reward regions in the pathogenesis and maintenance of BED. To date, the efficacy of various agents that target these and other neurotransmitter systems involved in motivated feeding behavior, mood regulation, and impulse control have been investigated in the treatment of BED. Several antidepressant and anticonvulsant agents have demonstrated efficacy in reducing binge eating frequency, but only in limited cases have these effects resulted in patients achieving abstinence, which is the primary goal of treatment; they also range from less (fluvoxamine) to more (topiramate) effective in achieving weight loss that is both clinically meaningful and significantly greater than placebo. Collectively, the literature on pharmacological treatment approaches to BED is limited in that very few agents have been studied in multiple, confirmatory trials with adequate follow up, and almost none have been evaluated in large patient samples that are diverse with respect to age, sex, and ethnicity. In addition, prior trials have not adequately addressed, through study design, the high placebo response commonly observed in this patient population. Several novel agents are in various phases of testing, and recent animal studies focusing on glutamate-signaling circuits linking the amygdala to the lateral hypothalamus offer new avenues for exploration and potential therapeutic development. Studies of newly FDA-approved medications for long-term obesity treatment and further explorations of dietary supplements and neutraceuticals with appetite- and mood-altering properties may also be worthwhile.
机译:在美国,狂暴的饮食障碍(床)是最常见的饮食障碍,终身患病率类似于成年女性的3.5%,成人男性2.0%,青少年中1.6%。床的特点是频繁的狂犬病剧集,伴随着对进食的控制丧失和导致心理困扰的丧失感。床是高度肥胖,抑郁症和其他精神病条件的高度持久性,它与实质性损害有关。目前,没有美国FDA批准的药理学治疗床。动物和人类研究涉及多巴胺,阿片类药物,乙酰胆碱和血清素神经核衣物在脑奖励区域内的多巴胺,阿片类药物,血清素神经系列中的潜在的丧失抑制。迄今为止,在床的治疗中已经研究了靶向涉及动力的饲养行为,情绪调节和脉冲控制的各种神经递质系统的疗效。几种抗抑郁药和抗惊厥药具有降低狂犬病频率的疗效,但只有在有限的情况下,这些效果导致患者实现禁欲的患者,这是治疗的主要目标;它们的范围从较少(Fluvoxamine)到更多(Topiramate)有效地实现了临床上有意义,并且明显大于安慰剂。统称,对药理治疗方法的文献是有限的,因为已经在多种验证性试验中研究了很少的药剂,并且几乎没有人在多元化的大型患者样本中进行评估,这是对年龄,性别不同的,和种族。此外,通过研究设计,在本患者群体中通常观察到的高安慰剂反应没有充分解决先前的试验。几种新药处于各种阶段的测试,最近的动物研究重点是将杏仁盐的谷氨酸信号通信电路连接到侧丘脑,为侧丘脑提供了新的途径,用于勘探和潜在的治疗发育。对新型FDA批准的长期肥胖治疗药物的研究以及膳食补充剂和中型物品的进一步探索和情绪改变的性质也可能是值得的。

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