Department of Biological Science, 319 Stadium Drive, Suite 3008, King Life Sciences Building, The Florida State University, Tallahassee, FL 32306-4295, United States; Program in Neuroscience, 319 Stadium Drive, Suite 3008, King Life Sciences Building, The Florida State University, Tallahassee, FL 32306-4295, United States.
Physiol Behav. 2012 Oct 10;107(3):424-32. doi: 10.1016/j.physbeh.2012.09.007. Epub 2012 Sep 17.
Physiological and nutritional state can modify sensory ability and perception through hormone signaling. Obesity and related metabolic disorders present a chronic imbalance in hormonal signaling that could impact sensory systems. In the olfactory system, external chemical cues are transduced into electrical signals to encode information. It is becoming evident that this system can also detect internal chemical cues in the form of molecules of energy homeostasis and endocrine hormones, whereby neurons of the olfactory system are modulated to change animal behavior towards olfactory cues. We hypothesized that chronic imbalance in hormonal signaling and energy homeostasis due to obesity would thereby disrupt olfactory behaviors in mice. To test this idea, we utilized three mouse models of varying body weight, metabolic hormones, and visceral adiposity - 1) C57BL6/J mice maintained on a condensed-milk based, moderately high-fat diet (MHF) of 32% fat for 6 months as the diet-induced obesity model, 2) an obesity-resistant, lean line of mice due to a gene-targeted deletion of a voltage-dependent potassium channel (Kv 1.3-null), and 3) a genetic model of obesity as a result of a gene-targeted deletion of the melanocortin 4 receptor (MC4R-null). Diet-induced obese (DIO) mice failed to find a fatty-scented hidden peanut butter cracker, based solely on olfactory cues, any faster than an unscented hidden marble, initially suggesting general anosmia. However, when these DIO mice were challenged to find a sweet-scented hidden chocolate candy, they had no difficulty. Furthermore, DIO mice were able to discriminate between fatty acids that differ by a single double bond and are components of the MHF diet (linoleic and oleic acid) in a habituation-dishabituation paradigm. Obesity-resistant, Kv1.3-null mice exhibited no change in scented object retrieval when placed on the MHF-diet, nor did they perform differently than wild-type mice in parallel habituation-dishabituation paradigms of fatty food-related odor components. Genetically obese, MC4R-null mice successfully found hidden scented objects, but did so more slowly than lean, wild-type mice, in an object-dependent fashion. In habituation-dishabituation trials of general odorants, MC4R-null mice failed to discriminate a novel odor, but were able to distinguish two fatty acids. Object memory recognition tests for short- and long-term memory retention demonstrated that maintenance on the MHF diet did not modify the ability to perform these tasks independent of whether mice became obese or were resistant to weight gain (Kv1.3-null), however, the genetically predisposed obese mice (MC4R-null) failed the long-term object memory recognition performed at 24h. These results demonstrate that even though both the DIO mice and genetically predisposed obese mice are obese, they vary in the degree to which they exhibit behavioral deficits in odor detection, odor discrimination, and long-term memory.
生理和营养状态可以通过激素信号来改变感觉能力和感知。肥胖和相关的代谢紊乱会导致激素信号的慢性失衡,从而影响感觉系统。在嗅觉系统中,外部化学线索被转化为电信号以编码信息。现在越来越明显的是,这个系统还可以检测到内部化学线索,形式为能量稳态和内分泌激素的分子,由此,嗅觉系统的神经元被调节以改变动物对嗅觉线索的行为。我们假设肥胖引起的激素信号和能量稳态的慢性失衡会因此破坏小鼠的嗅觉行为。为了验证这一观点,我们利用了三种体重、代谢激素和内脏肥胖程度不同的小鼠模型-1)C57BL6/J 小鼠在 32%脂肪的浓缩牛奶基础上高脂饮食 6 个月作为饮食诱导肥胖模型,2)一种由于电压依赖性钾通道(Kv1.3)的基因靶向缺失而肥胖抵抗的瘦线,和 3)一种由于黑素皮质素 4 受体(MC4R)的基因靶向缺失而肥胖的遗传模型。饮食诱导肥胖(DIO)小鼠无法仅通过嗅觉线索找到有香味的隐藏花生酱饼干,与无香味的隐藏大理石相比,它们的速度没有任何提高,最初表明有普遍的嗅觉障碍。然而,当这些 DIO 小鼠被要求找到有香味的隐藏巧克力糖果时,它们没有任何困难。此外,DIO 小鼠能够在习惯化-去习惯化范式中区分出仅相差一个双键且是 MHF 饮食成分的脂肪酸(亚油酸和油酸)。肥胖抵抗性、Kv1.3 缺失的小鼠在接受 MHF 饮食时,在寻找有香味的物体方面没有变化,也没有像在肥胖相关气味成分的平行习惯化-去习惯化范式中与野生型小鼠表现出不同。遗传性肥胖、MC4R 缺失的小鼠成功地找到了隐藏的有香味的物体,但与瘦的野生型小鼠相比,它们的速度较慢,这是一种物体依赖的方式。在一般气味的习惯化-去习惯化试验中,MC4R 缺失的小鼠无法区分新的气味,但能够区分两种脂肪酸。对短期和长期记忆保留的物体记忆识别测试表明,维持 MHF 饮食不会改变执行这些任务的能力,无论小鼠是否肥胖或对体重增加有抵抗力(Kv1.3 缺失),然而,遗传上易患肥胖的小鼠(MC4R 缺失)在 24 小时后无法进行长期的物体记忆识别。这些结果表明,尽管 DIO 小鼠和遗传上易患肥胖的小鼠都肥胖,但它们在嗅觉检测、嗅觉辨别和长期记忆方面表现出行为缺陷的程度不同。