4.3 Article

Neurobiology of Avoidant/Restrictive Food Intake Disorder in Youth with Overweight/Obesity Versus Healthy Weight

期刊

出版社

ROUTLEDGE JOURNALS, TAYLOR & FRANCIS LTD
DOI: 10.1080/15374416.2021.1894944

关键词

Avoidant; restrictive food intake disorder; ARFID; functional magnetic resonance imaging; fMRI; reward; orbitofrontal cortex

资金

  1. National Institute of Mental Health [K24MH120568, R01MH108595]
  2. Nutrition and Obesity Research Center at Harvard [P30DK04056]
  3. Harvard Clinical and Translational Science Center [0UL1TR00110201]
  4. Pediatric Endocrine Society

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This study found that adolescents with avoidant/restrictive food intake disorder (ARFID) and overweight/obesity (OV/OB) demonstrate hyperactivation in brain regions critical for the reward value of food cues compared to those with healthy weight (HW). Postprandial changes in subjective hunger are dependent on BMI and mediated by activation in the orbitofrontal cortex (OFC). These neurobiological differences may contribute to selective overeating in individuals with ARFID and OV/OB and could potentially be targeted in treatment.
Objective: Avoidant/restrictive food intake disorder (ARFID) occurs across the weight spectrum, however research addressing the coexistesnce of ARFID with overweight/obesity (OV/OB) is lacking. We aimed to establish co-occurrence of OV/OB and ARFID and to characterize divergent neurobiological features of ARFID by weight. Method: Youth with full/subthreshold ARFID (12 with healthy weight [HW], 11 with OV/OB) underwent fasting brain fMRI scan while viewing food/non-food images (M age = 16.92 years, 65% female, 87% white). We compared groups on BOLD response to high-calorie foods (HCF) (vs. objects) in food cue processing regions of interest. Following fMRI scanning, we evaluated subjective hunger pre- vs. post-meal. We used a mediation model to explore the association between BMI, brain activation, and hunger. Results: Participants with ARFID and OV/OB demonstrated significant hyperactivation in response to HCF (vs. objects) in the orbitofrontal cortex (OFC) and anterior insula compared with HW participants with ARFID. Mediation analysis yielded a significant indirect effect of group (HW vs. OV/OB) on hunger via OFC activation (effect = 18.39, SE = 11.27, 95% CI [-45.09, -3.00]), suggesting that OFC activation mediates differences in hunger between ARFID participants with HW and OV/OB. Conclusions: Compared to youth with ARFID and HW, those with OV/OB demonstrate hyperactivation of brain areas critical for the reward value of food cues. Postprandial changes in subjective hunger depend on BMI and are mediated by OFC activation to food cues. Whether these neurobiological differences contribute to selective hyperphagia in ARFID presenting with OV/OB and represent potential treatment targets is an important area for future investigation.

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