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The hunger games: taste, GLP-1 and female gender involved P-0449 (CROSBI ID 657989)

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Baretić, Maja ; Kušec, Vesna ; Uroić, Valentina, Pavlić-Renar, Ivana ; Altabas, Velimir The hunger games: taste, GLP-1 and female gender involved P-0449 // IDF Congress 2017: International Diabetes Federation Abu Dhabi, Ujedinjeni Arapski Emirati, 04.12.2017-08.12.2017

Podaci o odgovornosti

Baretić, Maja ; Kušec, Vesna ; Uroić, Valentina, Pavlić-Renar, Ivana ; Altabas, Velimir

engleski

The hunger games: taste, GLP-1 and female gender involved P-0449

Background The crucial role of the gustatory system during evolution was to detect potentially toxic nutrients or to detect indicators of spoilage. As the human brain evolved and body volume increased, tooth and gut size decreased. Nutritional characteristics also evolved in conjunction with the high metabolic demand of large brains. Incretins are substances secreted in the gut after a meal. The incretin hormone glucagon-like peptide-1 (GLP-1) is released from intestinal enteroendocrine L cells in response to a carbohydrate meal. GLP-1 has many levels of action, but currently it is primarily known for its effect on beta cells. GLP-1 reduces gastric emptying, lowers appetite by promoting satiety via hypothalamic receptors and reduces food intake. Thus, GLP-1 action leads to weight loss. GLP-1 is produced not only in the peripheral nervous system (intestine and pancreas) but also in the central nervous system by neurons located in the nucleus of the solitary tract. Central injections of GLP-1 receptor agonists decrease food intake. There is no specific group of diabetic (or non- diabetic) patients identified as GLP-1 receptor agonist 'responders” or 'non- responders” with respect to weight loss. Some patients report a diminished craving for food following GLP-1 therapy and a change in food preference. Aim The gastrointestinal tract is the major connector between food and body weight, it senses basic tastes in a similar manner as the tongue and through similar G-protein-coupled taste receptors. The link between gut hormones and eating behavior is well known, though it has not been thoroughly explored. The aim of this study was to explore how GLP-1 influences taste preference in different genders, insulin sensitivity and body composure. Method Effects of GLP-1 infusion on taste preference were investigated in 14 healthy participants (6 males, 8 females) in a double- blind, placebo- controlled crossover study. Insulin sensitivity was estimated with simultaneously measured fasting plasma glucose and fasting plasma insulin values and body composition was estimated with bioelectrical impedance analysis (total fat mass, mean fat percentage). After an overnight fast and an oral sodium load delivered in the form of soup, volunteers received placebo (500 ml of 0.9% saline) over a 3-hour period. At the end of infusion, participants chose their current food preferences from illustrations of food types representing 5 tastes (sweet, bitter, salty, sour, and umami). After 7 days, the volunteers received an infusion of synthetic GLP-1 (1.5 pmol/kg/min, dissolved in 500 ml of 0.9% saline) and reported their food preferences again. Results Change of taste preference after GLP-1 infusion but not after placebo was reported as response, and non-response was reported in the case of taste persistence. A statistically significant difference in response type was found between sexes (χ2= 4.667, df=1, p=0.031), with women being more likely to change their taste preference after GLP-1 infusion than men. There was a positive correlation in responders between the body composition parameter (body fat mass in kg) and basal insulin levels after GLP-1 infusion. We also found a strong positive correlation between insulin resistance and insulin level after GLP-1 infusion in responders (r= 0.89 p<0.01) Discussion The results of this study indicated that healthy non-obese women were more likely to change their taste preference after GLP-1 infusion than men. Why are women more prone to taste change after GLP-1 infusion than men? Observed change of taste upon GLP-1 infusion in women might be ascribed to estrogen ; the weight-lowering effects of estrogens are accomplished by receptor-mediated delivery. The weight-lowering effects of estrogens are associated with decreased food intake and increased energy expenditure in experimental animals, modulating energy expenditure and feeding behavior through leptin-like effects in the hypothalamus. Estrogens act directly on brain serotonin neurons. According to current findings and this study data, recently developed estrogen/GLP-1 medication may be a new strategy for obesity therapy. Also, a current obesity therapy, a GLP-1 receptor agonist, may be more effective (or applied in lower dosages) in females. Gender differences in the physiology of eating and response to GLP-1 stimuli may contribute to better understanding of human obesity and eating disorders. For patients with more visceral fat and higher insulin resistance, a GLP-1 receptor agonist could be more effective (or applied in lower dosages) for the treatment of diabetes.

Glucagon-like peptide-1 ; Hunger ; Estrogen

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Podaci o prilogu

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Podaci o skupu

IDF Congress 2017: International Diabetes Federation

poster

04.12.2017-08.12.2017

Abu Dhabi, Ujedinjeni Arapski Emirati

Povezanost rada

Kliničke medicinske znanosti, Nutricionizam