The potential effect of α7 nicotinic receptors modulation on palatable food-induced dependence-like behaviors

IF 3 3区 医学 Q2 PHARMACOLOGY & PHARMACY Saudi Pharmaceutical Journal Pub Date : 2024-07-04 DOI:10.1016/j.jsps.2024.102138
Alaa A. Alameen , Shakir D. AlSharari , Musaad A. Alshammari , M.I. Damaj , Y. Sari
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Abstract

Background

The recent global increase in obesity rates, coupled with excessive palatable food (PF) consumption, has become a serious societal concern. Literature indicates that rewarding PF, especially upon cessation, can lead to overeating, binge eating, and compulsive eating, potentially resulting in obesity. Challenges in dietary paradigms, alongside limitations in approved treatments for eating disorders and anti-obesity medications, underscore the need to explore novel targets. In this context, α7nAChR (alpha-7 nicotinic acetylcholine receptor) may serve as a promising therapeutic target in combating food dependence and obesity. The present study aims to assess the role of α7nAChR in palatable food-induced dependence-like behaviors.

Method

The study involved male C57BL/6J mice exposed to three different feeding paradigms over 6 weeks to induce obesity and food addiction. On day 43, palatable food was replaced with standard chow, and the mice received treatments (vehicle, PNU-282987 [α7nAChR agonist], or methyllycaconitine citrate [MLA; α7nAChR antagonist]). Addiction-like behaviors, including craving for palatable food, motivation-effort interaction tests, and compulsive eating-like behavior, were measured during abstinence with and without treatment.

Results

The present study shows that chronic intermittent and continuous exposure to palatable food induces craving, motivation, and effort interaction behaviors as well as compulsive eating-like behaviors in palatable food-abstinent mice. Administration of the α7nAChR agonist, PNU-282987, significantly attenuated the craving behavior only in mice continuously fed palatable food (reduced calorie intake from 63.19 % to 48.21 %; p = 0.0053). Also, PNU-282987 suppressed the effort behaviors in either intermittently or continuously fed mice (significant reduction in the Δ number of active events per minute; p-values = 0.038 and 0.0098, respectively). However, it attenuated the compulsive-like eating behavior exclusively in the continuously fed group (p = 0.0433). Active and total interaction efforts were reversed by the MLA. These findings indicate the involvement of α7nAChR in dependence-like behaviors toward palatable food in mice.

Conclusion

Our findings demonstrate that dependence-like behaviors toward palatable food can emerge after prolonged exposure. Mice fed on palatable food continuously exhibited more dependence-like behaviors toward palatable food, and activation of α7nAChR signaling attenuated the vulnerability to develop such behaviors.

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调节α7烟碱受体对美味食物诱发的类似依赖行为的潜在影响
背景近年来,全球肥胖率上升,再加上适口食物(PF)消费过多,已成为一个严重的社会问题。文献表明,奖励性适口食物(尤其是在停止食用时)会导致暴饮暴食、暴饮暴食和强迫性进食,从而可能导致肥胖。饮食范式面临的挑战,以及已获批准的饮食失调症治疗方法和抗肥胖药物的局限性,凸显了探索新靶点的必要性。在这种情况下,α7nAChR(α-7 尼古丁乙酰胆碱受体)可能成为对抗食物依赖和肥胖症的一个有希望的治疗靶点。本研究旨在评估α7nAChR在适口食物诱导的类似依赖行为中的作用。第43天,用标准饲料取代适口食物,小鼠接受治疗(载体、PNU-282987[α7nAChR激动剂]或柠檬酸甲酯[MLA;α7nAChR拮抗剂])。结果本研究表明,长期间歇性和持续暴露于适口食物会诱发成瘾小鼠的渴求、动机和努力相互作用行为以及强迫性进食行为。服用α7nAChR激动剂PNU-282987仅能显著减轻连续喂食适口食物的小鼠的渴求行为(卡路里摄入量从63.19%降至48.21%;p = 0.0053)。此外,PNU-282987 还能抑制间歇或连续喂食小鼠的努力行为(显著减少每分钟活动事件的 Δ 数量;p 值分别为 0.038 和 0.0098)。然而,它只减轻了连续喂食组的强迫性进食行为(p = 0.0433)。主动和全面的交互作用被 MLA 逆转。这些研究结果表明,α7nAChR 参与了小鼠对适口食物的依赖行为。连续喂食适口食物的小鼠对适口食物表现出更多类似依赖的行为,而激活α7nAChR信号转导可减轻出现此类行为的脆弱性。
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来源期刊
Saudi Pharmaceutical Journal
Saudi Pharmaceutical Journal PHARMACOLOGY & PHARMACY-
CiteScore
6.10
自引率
2.40%
发文量
194
审稿时长
67 days
期刊介绍: The Saudi Pharmaceutical Journal (SPJ) is the official journal of the Saudi Pharmaceutical Society (SPS) publishing high quality clinically oriented submissions which encompass the various disciplines of pharmaceutical sciences and related subjects. SPJ publishes 8 issues per year by the Saudi Pharmaceutical Society, with the cooperation of the College of Pharmacy, King Saud University.
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