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北京大学学报(医学版) ›› 2016, Vol. 48 ›› Issue (5): 777-782. doi: 10.3969/j.issn.1671-167X.2016.05.005

• 论著 • 上一篇    下一篇

尼古丁减轻高脂高果糖诱导的非酒精性脂肪性肝炎小鼠的肝脏炎症

陈小梅1,李富强1,严速2,吴小翠1,唐翠兰1△   

  1. (1. 浙江中医药大学附属第二医院肝病科, 杭州310005; 2. 温州医科大学附属第一医院腔镜外科, 浙江温州325000)
  • 出版日期:2016-10-18 发布日期:2016-10-18
  • 通讯作者: 唐翠兰 E-mail:1747603542@qq.com
  • 基金资助:

    国家自然科学基金(81100279)和浙江省新苗人才计划项目(2014R410058)资助

Nicotine alleviates the liver inflammation of non-alcoholic steatohepatitis induced by high-fat and high-fructose in mice

CHEN Xiao-mei1, LI Fu-qiang1, YAN Su2, WU Xiao-cui1, TANG Cui-lan1△   

  1. (1. Department of Liver Disease, The Second Affiliated Hospital, Zhejiang Chinese Medical University, Hangzhou 310005, China; 2. Department of Endoscopic Surgery, The First Affiliated Hospital of Whenzhou Medical University, Wenzhou 325000, Zhejiang, China)
  • Online:2016-10-18 Published:2016-10-18
  • Contact: TANG Cui-lan E-mail:1747603542@qq.com
  • Supported by:

    Supported by the National Natural Science Foundation of China (81100279) and Xin-miao Talent Program of Zhejiang Province (2014R410058)

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摘要:

目的:探讨活化胆碱能抗炎通路对非酒精性脂肪性肝炎(nonalcoholic steatohepatitis,NASH)模型小鼠肝脏炎症的抑制作用及其分子机制。方法:60只雄性6周龄的无特定病原体(specific pathogen free,SPF)级C57BL/6J小鼠被随机分为4组:正常饮食小鼠生理盐水注射组、正常饮食小鼠尼古丁注射组、NASH模型小鼠生理盐水注射组和NASH模型小鼠尼古丁注射组,分别给予普通饮食及高脂饮食加高果糖饮水,喂养17周后建立NASH小鼠模型,然后予各组小鼠生理盐水或尼古丁腹腔注射,每天1次,注射量为400 μg/kg,注射3周。3周后处死动物进行肝组织病理检查,取小鼠血清行酶联免疫吸附测定(enzyme linked immunosorbent assay,ELISA)检测炎症因子白细胞介素-6(interleukin-6,IL-6)和肿瘤坏死因子-α(tumor necrosis factor-α,TNF-α),同时原代分离培养肝巨噬细胞,使用Western blot和荧光共聚焦显微镜检测α7尼古丁型乙酰胆碱能受体(alpha 7 nicotinic acetylcholine receptors,α7nAChR)、Toll样受体-4(Toll-like receptors-4,TLR-4)和磷酸化核转录因子-κB(nuclear factor κB of phosphorylation,p-NF-κB)的蛋白水平。结果:成功建立了NASH小鼠模型。给予小鼠尼古丁治疗后,小鼠肝组织病理结果显示,小鼠肝脏炎症和脂肪变性明显减轻;ELISA结果显示,小鼠血清中炎症因子IL-6、TNF-α水平下降;Western blot和荧光共聚焦显微镜结果显示,尼古丁治疗组小鼠α7nAChR蛋白水平上调,p-NF-κB水平下调。结论:活化胆碱能抗炎通路可以通过抑制NF-κB通路减轻NASH小鼠的肝脏炎症。

关键词: 尼古丁, 非酒精性脂肪性肝病, 受体, 胆碱能, 炎症介导素类, 小鼠

Abstract:

Objective:To investigate the anti-inflammation effects by activation of the cholinergic anti-inflammatory pathway and its mechanisms in non-alcoholic steatohepatitis (NASH) model mice. Me-thods: 6-week-old male C57BL/6J (B6) mice were randomly divided into four groups: the first group was normal mice, injected with saline; the second group was normal mice, injected with nicotine; the third group was NASH model mice, injected with saline; the fourth group was NASH model mice, injected with nicotine. The experimental mice were fed with either standard chow (SC) or high-fat and high-fructose (HFHF) for 17 weeks to generate an NASH model mice. The mice received injection once daily for 3 weeks [nicotine dose, 400 μg/kg]. Then, their pathological characteristics and function of the liver were assessed. The expressions of interleukin-6 (IL-6) and tumor necrosis factor-α (TNF-α) in serum were analyzed by enzyme linked immunosorbent assay (ELISA). The expressions of alpha 7 nicotinic acetylcholine receptors (α7nAChR), Toll-like receptors-4 (TLR-4) and nuclear factor κB of phosphory-lation (p-NF-κB) in Kupffer cells were determined by Western blot and immunofluorescence assays. Results: We successfully generated NASH model mice by imitating the high-fat and high-fructose dietary style of NASH patients. The results of our investigation demonstrated that nicotine could reduce significantly the levels of IL-6, and TNF-α in serum (P<0.05). The expression of p-NF-κB protein in the group which was NASH model mice injected with nicotine declined significantly as compared with the group which was NASH model mice injected with saline (P<0.05). And the expression of α7nAChR protein elevated significantly conversely (P<0.05). Conclusion: Activation of the cholinergic anti-inflammatory pathway could inhibit the release of inflammatory factors as TNF-α and IL-6 in NASH model mice, and the mechanism for the inhibition of inflammatory was mediated by NF-κB pathway.

Key words: Nicotine, Non-alcoholic fatty liver disease, Receptors, cholinergic, Inflammation mediators, Mice

中图分类号: 

  • R575.1
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ISSN 1671-167X
CN 11-4691/R
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