高脂饮食削弱了雄性而非雌性小鼠应激引起的摄食量减少和 Glp1r 背外侧隔区神经元的激活。

High fat diet blunts stress-induced hypophagia and activation of Glp1r dorsal lateral septum neurons in male but not in female mice.

机构信息

Department of Molecular Physiology & Biophysics, Vanderbilt University School of Medicine, 2215 Garland Avenue, Nashville, TN 37232, USA.

Department of Molecular Physiology & Biophysics, Vanderbilt University School of Medicine, 2215 Garland Avenue, Nashville, TN 37232, USA; Vanderbilt Center for Addiction Research, Vanderbilt University School of Medicine, 2215 Garland Avenue, Nashville, TN 37232, USA.

出版信息

Mol Metab. 2022 Oct;64:101571. doi: 10.1016/j.molmet.2022.101571. Epub 2022 Aug 8.

DOI:10.1016/j.molmet.2022.101571

PMID:35953023

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9418981/

Abstract

OBJECTIVE

While stress typically reduces caloric intake (hypophagia) in chow-fed rodents, presentation of palatable, high calorie substances during stress can increase caloric consumption (i.e. "comfort feeding") and promote obesity. However, little is known about how obesity itself affects feeding behavior in response to stress and the mechanisms that can influence stress-associated feeding in the context of obesity.

METHODS

We assessed food intake and other metabolic parameters in lean and obese male and female mice following acute restraint stress. We also measured real-time activity of glucagon-like peptide-1 (Glp1) receptor (Glp1r)-expressing neurons in the dorsal lateral septum (dLS) during stress in lean and obese mice using fiber photometry. Glp1r activation in various brain regions, including the dLS, promotes hypophagia in response to stress. Finally, we used inhibitory Designer Receptors Activated Exclusively by Designer Drugs (DREADDs) to test whether activation of Glp1r-expressing neurons in the LS is required for stress-induced hypophagia.

RESULTS

Lean male mice display the expected hypophagic response following acute restraint stress, but obese male mice are resistant to this acute stress-induced hypophagia. Glp1r-positive neurons in the dLS are robustly activated during acute restraint stress in lean but not in obese male mice. This raises the possibility that activation of dLS Glp1r neurons during restraint stress contributes to subsequent hypophagia. Supporting this, we show that chemogenetic inhibition of LS Glp1r neurons attenuates acute restraint stress hypophagia in male mice. Surprisingly, we show that both lean and obese female mice are resistant to acute restraint stress-induced hypophagia and activation of dLS Glp1r neurons.

CONCLUSIONS

These results suggest that dLS Glp1r neurons contribute to the hypophagic response to acute restraint stress in male mice, but not in female mice, and that obesity disrupts this response in male mice. Broadly, these findings show sexually dimorphic mechanisms and feeding behaviors in lean vs. obese mice in response to acute stress.

摘要

目的

尽管压力通常会减少 Chow 喂养啮齿动物的热量摄入（食欲减退），但在压力下呈现美味、高热量的物质会增加热量消耗（即“舒适喂养”）并促进肥胖。然而，对于肥胖本身如何影响应激反应中的进食行为以及在肥胖背景下影响与应激相关的进食的机制知之甚少。

方法

我们在急性束缚应激后评估了瘦鼠和肥胖雄性和雌性小鼠的食物摄入量和其他代谢参数。我们还使用光纤光度法测量了瘦鼠和肥胖鼠在应激期间外侧隔区（dLS）中胰高血糖素样肽-1（Glp1）受体（Glp1r）表达神经元的实时活性。各种脑区（包括 dLS）中 Glp1r 的激活可促进应激时的食欲减退。最后，我们使用抑制性 Designer Receptors Activated Exclusively by Designer Drugs（DREADDs）来测试 LS 中 Glp1r 表达神经元的激活是否是应激诱导的食欲减退所必需的。

结果

瘦雄性小鼠在急性束缚应激后表现出预期的食欲减退反应，但肥胖雄性小鼠对此急性应激诱导的食欲减退具有抵抗力。在瘦鼠中，外侧隔区（dLS）中的 Glp1r 阳性神经元在急性束缚应激期间被强烈激活，但在肥胖雄性小鼠中则不然。这使得在束缚应激期间 LS Glp1r 神经元的激活有助于随后的食欲减退成为可能。支持这一点，我们表明 LS Glp1r 神经元的化学遗传抑制可减轻雄性小鼠急性束缚应激的食欲减退。令人惊讶的是，我们发现瘦鼠和肥胖雌性小鼠都对急性束缚应激诱导的食欲减退和 dLS Glp1r 神经元的激活具有抵抗力。