Abstract

IntroductionBrain-derived neurotrophic factor (BDNF), as well as oxytocin (OXY), are centrally secreted neuropeptides regulating a range of physiological processes, including food intake and metabolism. Moreover, numerous reports suggest their role in affective and cognitive symptoms of various psychiatric disorders. Thus, the study aimed to measure the serum level of BDNF and its receptor—tropomyosin-related kinase B (TrkB) and OXY in the malnourished anorexia nervosa patients and following partial weight-recovery. The correlations between levels of these proteins with the primary symptoms of the anorexia nervosa (AN) were also analyzed.MethodologyEighty-four adolescent AN patients were recruited into the study, but only forty-two AN patients completed it. The control group comprises of thirty age- and height-matched girls (CG). Serum BDNF, TrkB, and OXY levels were measured in AN group in two time-points—at the beginning of the hospitalization in malnourished patients (AN-T1) and again after partial weight normalization, on the day of discharge (AN-T2). The severity of eating disorders, as well as depressive and obsessive-compulsive symptoms, were assessed at the same two-time points.ResultsBody mass index (BMI) differed significantly between the AN-T1, AN-T2, and CG. BDNF levels for the AN-T2 increased significantly in comparison to the AN-T1, but at two-time points were significantly lower than in the CG. The OXY level did not change with weight gain and in both groups AN-T1 and AN-T2 were statistically significantly higher than in the CG. Statistically significant negative correlations between BDNF and the severity of eating disorders symptoms were found. Depressive and obsessive-compulsive symptoms did not show significant correlations with levels of studied proteins for either malnourished or partially weight recovered AN patients.ConclusionsBDNF serum levels were decreased in the malnourished AN patients and tended to normalize with partial weight recovery. OXY serum levels were found to be increased in the malnourished AN patients and did not normalize with partial weight recovery, confirming previous reports about its role in the etiopathogenesis of AN. BDNF can be related to aberrant eating behaviors occurring in AN. Our results do not support the role of serum levels of BDNF, TrkB, or OXY in the modulation of depressive or obsessive-compulsive symptoms.

Highlights

  • Brain-derived neurotrophic factor (BDNF), as well as oxytocin (OXY), are centrally secreted neuropeptides regulating a range of physiological processes, including food intake and metabolism

  • We investigated the correlations between level of proteins and several symptomatic dimensions of anorexia nervosa (AN), namely eating disorder, depression, and obsessive-compulsive symptoms

  • BDNF serum concentration was lower in the malnourished AN patients and tended to normalize its level with weight gain

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Summary

Introduction

Brain-derived neurotrophic factor (BDNF), as well as oxytocin (OXY), are centrally secreted neuropeptides regulating a range of physiological processes, including food intake and metabolism. Oxytocin (OXY) is a nine-amino acid neuropeptide and neuromodulator mainly produced in the paraventricular nucleus (PVN) [6] and the supraoptic nucleus (SON) [7], which primarily regulates reproductive behaviors and mother– infant interactions [8] It is released into the bloodstream, entering peripheral circulation, as well as directly into the nervous system [9]. If obesity was associated with diabetes the serum OXY levels were decreased [18] In both healthy-weight and obese subjects, OXY administration can cause a reduction in caloric intake and consumption of palatable snacks [19], as well as improved glucose and lipid metabolism [20, 21]. The above results support the interest in the role of OXY as an anorexigenic factor both in healthy humans and patients suffering from eating disorders

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