N М Bazhan, T V Jakovleva, A Yu Kazantseva, N E Kostina, P E Orlov, N Yu Balybina, K О Baranov, E N Makarova
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引用次数: 0
Abstract
In animals, obesity caused by consumption of a sweet-fat diet (SFD) is the most adequate mouse model of human diet-induced obesity. Fibroblast growth factor 21 (FGF21) reduces body weight, beneficially affects taste preferences, and corrects glucose metabolism in obese mice. Sex is known to influence FGF21 effects in different models of diet-induced and hereditary obesity. In mice with SFD-induced obesity, the effects of FGF21 have been studied only in males. The aim of this study was to compare the effects of FGF21 on body weight, food preferences and glucose and lipid metabolism in C57Bl/6J male and female mice with SFD-induced obesity. Mice were fed with a diet consisting of standard chow, lard and cookies for 10 weeks, then they were injected with FGF21 (1 mg per 1 kg) or vehicle for 7 days. Body weight, weights of different types of food, blood parameters, glucose tolerance, gene and protein expression in the liver, gene expression in the white, brown adipose tissues, and the hypothalamus were assessed. FGF21 administration reduced body weight, did not alter total energy consumption, and activated orexigenic pathways of hypothalamus in mice of both sexes. However, sex dimorphism was found in the realization of the orexigenic FGF21 action at the transcriptional level in the hypothalamus. Metabolic effects of FGF21 were also sex-specific. Only in males, FGF21 exerted beneficial antidiabetic action: it reduced fatty acid and leptin plasma levels, improved glucose-tolerance, and upregulated hepatic expression of Ppargc1, Fasn, Accα, involved in lipid turnover, gene Insr and protein glucokinase, involved in insulin action. Only in obese females, FGF21 induced preference of standard diet to sweet food. Thus, in mouse model of obesity induced by consumption of a sweet-fat diet, the catabolic effect of FGF21 was not sex-specific and hormonal, transcriptional and behavioral effects of FGF21 were sex-specific. These data suggest elaboration of different approaches to use FGF21 analogs for correction of metabolic consequences of obesity in different sexes.
在动物中,由食用甜脂饮食引起的肥胖是人类饮食引起的肥胖的最适当的小鼠模型。成纤维细胞生长因子21 (FGF21)可以减轻肥胖小鼠的体重,有益地影响味觉偏好,并纠正葡萄糖代谢。已知性别会影响FGF21在不同饮食诱导和遗传性肥胖模型中的作用。在sfd诱导的肥胖小鼠中,FGF21的作用仅在雄性小鼠中进行了研究。本研究的目的是比较FGF21对sfd诱导肥胖C57Bl/6J雌雄小鼠体重、食物偏好和糖脂代谢的影响。小鼠以标准鼠粮、猪油和饼干组成的饮食喂养10周,然后注射FGF21(每1 kg 1 mg)或整车7天。评估体重、不同类型食物的体重、血液参数、葡萄糖耐量、肝脏基因和蛋白质表达、白色脂肪组织、棕色脂肪组织和下丘脑基因表达。FGF21降低了小鼠的体重,没有改变总能量消耗,并激活了下丘脑的供氧途径。然而,在下丘脑的转录水平上,FGF21的促氧作用的实现中发现了性别二态性。FGF21的代谢作用也具有性别特异性。仅在男性中,FGF21发挥了有益的降糖作用:它降低了脂肪酸和瘦素血浆水平,提高了葡萄糖耐量,上调了肝脏中参与脂质转换的Ppargc1、Fasn、Accα的表达,上调了参与胰岛素作用的基因Insr和蛋白葡萄糖激酶的表达。只有在肥胖女性中,FGF21诱导了标准饮食对甜食的偏好。因此,在食用甜脂饮食引起的肥胖小鼠模型中,FGF21的分解代谢作用不具有性别特异性,FGF21的激素、转录和行为效应具有性别特异性。这些数据表明,使用FGF21类似物来纠正不同性别肥胖的代谢后果的不同方法。
期刊介绍:
The "Vavilov Journal of genetics and breeding" publishes original research and review articles in all key areas of modern plant, animal and human genetics, genomics, bioinformatics and biotechnology. One of the main objectives of the journal is integration of theoretical and applied research in the field of genetics. Special attention is paid to the most topical areas in modern genetics dealing with global concerns such as food security and human health.