de Leeuw van Weenen J E, Parlevliet E T, Schröder-van der Elst J P, van den Berg S A, Willems van Dijk K, Romijn J A, Pijl H
Department of Endocrinology and Metabolic Diseases, Leiden University Medical Center, RC Leiden, The Netherlands.
Exp Diabetes Res. 2011;2011:928523. doi: 10.1155/2011/928523. Epub 2011 Apr 6.
High fat feeding induces a variety of obese and lean phenotypes in inbred rodents. Compared to Diet Resistant (DR) rodents, Diet Induced Obese (DIO) rodents are insulin resistant and have a reduced dopamine receptor D2 (DRD2) mediated tone. We hypothesized that this differing dopaminergic tone contributes to the distinct metabolic profiles of these animals. C57Bl6 mice were classified as DIO or DR based on their weight gain during 10 weeks of high fat feeding. Subsequently DIO mice were treated with the DRD2 agonist bromocriptine and DR mice with the DRD2 antagonist haloperidol for 2 weeks. Compared to DR mice, the bodyweight of DIO mice was higher and their insulin sensitivity decreased. Haloperidol treatment reduced the voluntary activity and energy expenditure of DR mice and induced insulin resistance in these mice. Conversely, bromocriptine treatment tended to reduce bodyweight and voluntary activity, and reinforce insulin action in DIO mice. These results show that DRD2 activation partly redirects high fat diet induced metabolic anomalies in obesity-prone mice. Conversely, blocking DRD2 induces an adverse metabolic profile in mice that are inherently resistant to the deleterious effects of high fat food. This suggests that dopaminergic neurotransmission is involved in the control of metabolic phenotype.
高脂喂养会在近交系啮齿动物中诱导出多种肥胖和消瘦表型。与饮食抵抗(DR)啮齿动物相比,饮食诱导肥胖(DIO)啮齿动物存在胰岛素抵抗,且多巴胺受体D2(DRD2)介导的张力降低。我们推测,这种不同的多巴胺能张力导致了这些动物不同的代谢特征。根据高脂喂养10周期间的体重增加情况,将C57Bl6小鼠分为DIO或DR。随后,对DIO小鼠用DRD2激动剂溴隐亭治疗,对DR小鼠用DRD2拮抗剂氟哌啶醇治疗2周。与DR小鼠相比,DIO小鼠体重更高,胰岛素敏感性降低。氟哌啶醇治疗降低了DR小鼠的自主活动和能量消耗,并在这些小鼠中诱导了胰岛素抵抗。相反,溴隐亭治疗倾向于降低DIO小鼠的体重和自主活动,并增强胰岛素作用。这些结果表明,DRD2激活部分地纠正了易肥胖小鼠中高脂饮食诱导的代谢异常。相反,阻断DRD2会在对高脂食物有害影响具有固有抗性的小鼠中诱导不良的代谢特征。这表明多巴胺能神经传递参与了代谢表型的控制。
