首页|期刊导航|陆军军医大学学报|司美格鲁肽通过调控炎症改善自闭症谱系障碍模型小鼠的核心症状

司美格鲁肽通过调控炎症改善自闭症谱系障碍模型小鼠的核心症状OA

Semaglutide ameliorates core symptoms in mouse model of autism spectrum disorder by regulating inflammation-related pathways

中文摘要英文摘要

目的 基于司美格鲁肽的神经保护与抗炎特性,本研究旨在探究其是否通过调控炎症相关靶点及信号通路,改善自闭症谱系障碍(autism spectrum disorder,ASD)模型小鼠BTBR T(+)Itpr3(tf)/J(BTBR)小鼠核心症状的作用途径与机制.方法 将32只7周龄雄性C57BL/6J(C57)与BTBR小鼠按随机数字表法随机分为4组(n=8);药物组腹腔注射25 nmol/kg司美格鲁肽,对照组注射生理盐水,连续干预7天,并且持续监测体质量.通过三箱、理毛、埋珠、新物体识别、Y迷宫、旷场行为学试验评估小鼠行为学指标,于行为学结束后,收取脑组织标本,并结合网络药理学、GO/KEGG富集分析、蛋白质-蛋白质相互作用分析、分子对接技术及qRT-PCR技术探究司美格鲁肽可能的作用机制.结果 司美格鲁肽干预7 d可显著降低BTBR小鼠的体质量(P<0.05),提升BTBR小鼠的三箱箱体偏好系数(P<0.01)、嗅探偏好系数(P<0.05)、新物体识别辨别系数(P<0.001),减少理毛(P<0.01)及埋珠(P<0.01)等重复刻板行为;但对C57小鼠的上述行为无显著影响,同时在旷场实验中显示对运动能力无明显影响.通过网络药理学分析,筛选出78个共同靶点,且这些靶点富集于炎症相关通路.结果 显示,司美格鲁肽与炎症相关通路中的可能靶点Serpine1、Mmp9、Pparg、Stat3、Ppara、Nr1h3等均具有良好的结合亲和力,结合能均≤-4 kcal/mol;qRT-PCR进一步证实,司美格鲁肽干预显著降低BTBR小鼠海马中Serpine1、Mmp9、Stat3、Il6、Tnfa、Il17a和Il1b mRNA的表达水平(P<0.05),上调Pparg的表达(P<0.05).结论 司美格鲁肽可通过调控神经炎症改善成年BTBR小鼠的自闭症样症状,为自闭症的临床治疗提供新的潜在药物靶点与实验依据.

Objective Based on the neuroprotective and anti-inflammatory properties of semaglutide,this study aims to investigate whether semaglutide improves core symptoms in BTBR T(+)Itpr3(tf)/J(BTBR)mice,a model of autism spectrum disorder(ASD),through modulation of inflammation-related targets and signaling pathways.Methods A total of 32 male C57BL/6J(C57)and BTBR mice(7 weeks old)were randomly divided into 4 groups(n=8):The treatment group received intraperitoneal injection of 25 nmol/kg semaglutide,while the control group received normal saline,with continuous intervention for 7 d,and body weight was monitored continuously throughout the intervention period.Mouse behavioral indicators were evaluated using various behavioral tests,including the three-chamber sociability test,grooming test,marble-burying test,novel object recognition test,Y-maze test and open field test.After behavioral assessments,the brain tissues were collected,and network pharmacology,GO/KEGG enrichment analysis,protein-protein interaction analysis,molecular docking technology,and qRT-PCR were employed to explore the potential mechanisms of semaglutide.Results Semaglutide intervention for 7 d significantly reduced the body weight of BTBR mice(P<0.05),increased the preference index from chamber time(P<0.01)and preference index from sniffing time(P<0.05),elevated the novel object recognition discrimination index(P<0.01),and reduced repetitive stereotyped behaviors such as self-grooming(P<0.001)and marble burying(P<0.01).However,no significant effects on the above mentioned behaviors were observed in C57 mice,and no obvious impact on locomotor activity was demonstrated in the open field test.Network pharmacology analysis identified 78 common targets which enriched in inflammation-related pathways.Semaglutide exhibited favorable binding affinity with potential targets in inflammation-related pathways including Serpine1,Mmp9,Pparg,Stat3,Ppara,and Nr1h3,with binding energies all≤-4 kcal/mol.qRT-PCR further confirmed that semaglutide intervention significantly downregulated mRNA expression levels of Serpine1,Mmp9,Stat3,Il6,Tnfa,Il17a,and Il1b(P<0.05),and upregulated Pparg expression(P<0.05)in the hippocampus of BTBR mice.Conclusion Semaglutide alleviates ASD-like symptoms in BTBR mice by regulating inflammation-related pathways,thus offering a promising potential treatment and foundational research for the clinical management of ASD.

刘嘉音;刘天曜;罗静;张星高;龚美凤;郭黎;范晓棠

陆军军医大学(第三军医大学)心理系军事认知心理学教研室,重庆陆军军医大学(第三军医大学)心理系军事认知心理学教研室,重庆陆军军医大学(第三军医大学)心理系军事认知心理学教研室,重庆陆军军医大学(第三军医大学)心理系军事认知心理学教研室,重庆陆军军医大学(第三军医大学)心理系军事认知心理学教研室,重庆陆军军医大学(第三军医大学)第一附属医院内分泌科,重庆陆军军医大学(第三军医大学)心理系军事认知心理学教研室,重庆

医药卫生

司美格鲁肽孤独症BTBR小鼠神经炎症

semaglutideautism spectrum disorderBTBR miceneuroinflammation

《陆军军医大学学报》 2026 (7)

882-894,13

国家自然科学基金面上项目(32471027) Supported by the General Program of National Natural Science Foundation of China(32471027).

10.16016/j.2097-0927.202601037

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