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享乐性进食的一种新生物标志物?对急性阿片类药物阻断的皮质醇和恶心反应的初步研究。

A new biomarker of hedonic eating? A preliminary investigation of cortisol and nausea responses to acute opioid blockade.

作者信息

Daubenmier Jennifer, Lustig Robert H, Hecht Frederick M, Kristeller Jean, Woolley Josh, Adam Tanja, Dallman Mary, Epel Elissa

机构信息

Osher Center for Integrative Medicine, Department of Medicine, University of California, San Francisco, United States.

Department of Pediatrics, University of California, San Francisco, United States.

出版信息

Appetite. 2014 Mar;74:92-100. doi: 10.1016/j.appet.2013.11.014. Epub 2013 Nov 27.

Abstract

Overweight and obese individuals differ in their degree of hedonic eating. This may reflect adaptations in reward-related neural circuits, regulated in part by opioidergic activity. We examined an indirect, functional measure of central opioidergic activity by assessing cortisol and nausea responses to acute opioid blockade using the opioid antagonist naltrexone in overweight/obese women (mean BMI=31.1±4.8) prior to the start of a mindfulness-based intervention to reduce stress eating. In addition, we assessed indices of hedonic-related eating, including eating behaviors (binge eating, emotional eating, external eating, restraint) and intake of sweets/desserts and carbohydrates (Block Food Frequency); interoceptive awareness (which is associated with dysregulated eating behavior); and level of adiposity at baseline. Naltrexone-induced increases in cortisol were associated with greater emotional and restrained eating and lower interoceptive awareness. Naltrexone-induced nausea was associated with binge eating and higher adiposity. Furthermore, in a small exploratory analysis, naltrexone-induced nausea predicted treatment response to the mindfulness intervention, as participants with more severe nausea at baseline maintained weight whereas those with little or no nausea responses tended to gain weight. These preliminary data suggest that naltrexone-induced cortisol release and nausea may help identify individuals who have greater underlying food reward dependence, which leads to an excessive drive to eat. Future research is needed to confirm this finding and to test if these markers of opioidergic tone might help predict success in certain types of weight management programs.

摘要

超重和肥胖个体在享乐性进食程度上存在差异。这可能反映了奖励相关神经回路的适应性变化,部分受阿片类活性调节。在一项基于正念的干预措施开始以减少压力性进食之前,我们通过使用阿片类拮抗剂纳曲酮评估超重/肥胖女性(平均BMI = 31.1±4.8)对急性阿片类阻断的皮质醇和恶心反应,来检测中枢阿片类活性的一种间接功能性指标。此外,我们评估了享乐性相关进食的指标,包括进食行为(暴饮暴食、情绪化进食、外在进食、克制)以及甜食/甜点和碳水化合物的摄入量(食物频率问卷);内感受性觉知(与失调的进食行为相关);以及基线时的肥胖程度。纳曲酮诱导的皮质醇增加与更多的情绪化和克制性进食以及更低的内感受性觉知相关。纳曲酮诱导的恶心与暴饮暴食和更高的肥胖程度相关。此外,在一项小型探索性分析中,纳曲酮诱导的恶心预测了对正念干预的治疗反应,因为基线时恶心更严重的参与者维持了体重,而那些恶心反应很少或没有的参与者往往体重增加。这些初步数据表明,纳曲酮诱导的皮质醇释放和恶心可能有助于识别那些潜在食物奖励依赖性更强的个体,这种依赖性会导致过度的进食冲动。需要进一步的研究来证实这一发现,并测试这些阿片类张力标记物是否有助于预测某些类型体重管理项目的成功。

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