Muelbl Matthew J, Nawarawong Natalie N, Clancy Patrick T, Nettesheim Catherine E, Lim Yi Wei, Olsen Christopher M
Neuroscience Research Center and Department of Pharmacology & Toxicology, Medical College of Wisconsin, 8701 Watertown Plank Road, Milwaukee, WI, 53226, USA.
Psychopharmacology (Berl). 2016 Jul;233(14):2799-811. doi: 10.1007/s00213-016-4323-9. Epub 2016 Jun 3.
Although leptin receptors are found in hypothalamic nuclei classically associated with homeostatic feeding mechanisms, they are also present in brain regions known to regulate hedonic-based feeding, natural reward processing, and responses to drugs of abuse. The ob/ob mouse is deficient in leptin signaling, and previous work has found altered mesolimbic dopamine signaling and sensitivity to the locomotor activating effects of amphetamine in these mice.
We directly assessed responses to three drugs of abuse and non-drug rewards in the leptin-deficient ob/ob mouse.
Ob/ob mice were tested in assays of sweet preference, novelty seeking, and drug reward/reinforcement.
In assays of novelty seeking, novel open field activity and operant sensation seeking were reduced in ob/ob mice, although novel object interaction and novel environment preference were comparable to wild types. We also found that ob/ob mice had specific phenotypes in regard to cocaine: conditioned place preference for 2.5 mg/kg was increased, while the locomotor response to 10 mg/kg was reduced, and cocaine self-administration was the same as wild types. Ob/ob mice also acquired self-administration of the potent opioid remifentanil, but breakpoints for the drug were significantly reduced. Finally, we found significant differences in ethanol drinking in ob/ob mice that correlated negatively with body weight and positively with operant sensation seeking.
In conclusion, ob/ob mice displayed task-specific deficits in novelty seeking and dissociable differences in reward/reinforcement associated with cocaine, remifentanil, and ethanol.
尽管瘦素受体存在于下丘脑核中,这些核传统上与稳态进食机制相关,但它们也存在于已知调节基于享乐的进食、自然奖赏处理以及对滥用药物反应的脑区。ob/ob小鼠存在瘦素信号缺陷,先前的研究发现这些小鼠中脑边缘多巴胺信号改变以及对苯丙胺的运动激活作用敏感性改变。
我们直接评估了瘦素缺乏的ob/ob小鼠对三种滥用药物和非药物奖赏的反应。
对ob/ob小鼠进行甜味偏好、新奇寻求以及药物奖赏/强化试验。
在新奇寻求试验中,ob/ob小鼠的新奇旷场活动和操作性感觉寻求减少,尽管新奇物体互动和新奇环境偏好与野生型相当。我们还发现ob/ob小鼠在可卡因方面有特定表型:对2.5mg/kg可卡因的条件性位置偏好增加,而对10mg/kg可卡因的运动反应减少,且可卡因自我给药与野生型相同。ob/ob小鼠也学会了自我给药强效阿片类药物瑞芬太尼,但该药物的断点显著降低。最后,我们发现ob/ob小鼠在乙醇饮用方面存在显著差异,这与体重呈负相关,与操作性感觉寻求呈正相关。
总之,ob/ob小鼠在新奇寻求方面表现出任务特异性缺陷,在与可卡因、瑞芬太尼和乙醇相关的奖赏/强化方面存在可分离的差异。
