高脂饮食加重小鼠肠易激综合征肠屏障损伤

doi:10.16352/j.issn.1001-6325.2025.08.1022

基础医学与临床 ›› 2025, Vol. 45 ›› Issue (8): 1022-1027.doi: 10.16352/j.issn.1001-6325.2025.08.1022

高脂饮食加重小鼠肠易激综合征肠屏障损伤

赵翠娟^*, 敖民, 武文博, 李妍华

内蒙古医科大学第三临床医学院(内蒙古包钢医院) 消化内科,内蒙古包头 014000

收稿日期:2024-06-26 修回日期:2024-11-11 出版日期:2025-08-05 发布日期:2025-07-11
通讯作者: ^*zcj2006125@163.com
基金资助:
内蒙古自治区科技计划项目(2022YFSH0042);航天医疗健康科技集团有限公司科研项目(2023YK22);内蒙古医学科学院公立医院科研联合基金科技项目(2023GLLH0242)

High fat diet aggravates intestinal barrier damage in mice with irritable bowel syndrome

ZHAO Cuijuan^*, AO Min, WU Wenbo, LI Yanhua

Department of Gastroenterology, Third Affiliated Hospital of Inner Mongolia Medical University(Inner Mongolia Baogang Hospital), Baotou 014000, China

Received:2024-06-26 Revised:2024-11-11 Online:2025-08-05 Published:2025-07-11
Contact: ^*zcj2006125@163.com

摘要/Abstract

摘要： 目的探究高脂饮食(HFD)对葡聚糖硫酸钠(DSS)诱导的肠易激综合征(IBS)小鼠肠屏障损伤和炎性反应的影响及潜在分子机制。方法将C57BL/6小鼠随机分为 4 组(n=6):正常组(normal组)、DSS组(饮用1.5% DSS溶液1周)、HFD+DSS组、HFD+DSS+WY14643组(每日腹腔注射PPARα激动剂WY14643 6 mg/kg)。观察小鼠体质量变化,测量肝脏重量,结肠HE染色观察病理,免疫组化法检测结肠胞质紧密黏连蛋白1(ZO-1)和闭锁蛋白(occludin)表达,qRT-PCR法测定结肠肿瘤坏死因子-ɑ(TNF-ɑ)、白细胞介素1-β(IL-1β)和白细胞介素-17(IL-17)mRNA表达,Western blot法测定结肠PPARα蛋白表达。结果 HFD+DSS组小鼠体质量与肝脏重量明显高于DSS组(均P＜0.001);HE染色显示正常组小鼠结肠组织结构正常,其余3组小鼠结肠黏膜出现不同程度损伤,可见少量炎性细胞浸润和上皮细胞脱落,其中HFD+DSS组肠黏膜损伤与炎性细胞浸润最严重,相较于DSS组,HFD+DSS组小鼠结肠中ZO-1、occludin蛋白表达降低(均P＜0.001),TNF-α、IL-1β、IL-17 mRNA表达升高(均P＜0.001),PPARα蛋白表达下调(P＜0.01);与HFD+DSS组相比,HFD+DSS+WY14643组肠黏膜损伤有所改善,炎性细胞浸润减轻,小鼠结肠ZO-1、Occludin蛋白表达增加(均P＜0.05),TNF-α、IL-1β、IL-17 mRNA表达下调(P＜0.01或P＜0.05),并且PPARα蛋白表达上调(P＜0.05)。结论 HFD诱导的肥胖可以加重IBS小鼠的肠黏膜病理损伤、肠屏障破坏及炎性反应,其分子机制与肠组织中PPARα表达下调相关。

关键词: 肠易激综合征, 肥胖, 过氧化物酶体增殖物激活受体α, 肠屏障损伤, 炎性因子

Abstract: Objective To explore the effects and underlying molecular mechanisms of high fat diet (HFD) on intestinal barrier damage and inflammatory reaction in mice with irritable bowel syndrome (IBS) induced by sodium dextran sulfate (DSS). Methods C57BL/6 mice were randomly divided into four groups (n=6): Normal group, DSS group (1.5% DSS solution for one week), HFD+DSS group, and HFD+DSS+WY14643 group(intraperitoneally injected daily with PPARα agonist WY14643 6 mg/kg). The body weight and liver weight of mice were measured. Colon pathology was observed by HE staining. The protein expression of zonula occludens-1(ZO-1) and occludin was detected by immunohistochemistry. The mRNA expression of tumor necrosis factor-α (TNF-α), interleukin-β (IL-1β), and interleukin-17 (IL-17) were determined by qRT-PCR. PPARα protein expression was determined by Western blot. Results The body weight and liver weight of mice in the HFD+DSS group were significantly higher than those in the DSS group (P＜0.001).HE staining showed normal colonic tissue structure in Normal group, while other three groups exhibited varying degrees of mucosal damage with a small amount of inflammatory cell infiltration and epithelial cell shedding. Among these, the HFD+DSS group displayed the most severe intestinal mucosal damage and inflammatory infiltration. Compared with the DSS group, the HFD+DSS group showed decreased ZO-1 and Occludin protein expression (P＜0.001), elevated TNF-α, IL-1 β, and IL-17 mRNA levels(all P＜0.001), and downregulated PPARα protein expression(P＜0.01).Compared with the HFD+DSS group, mice in HFD+DSS+WY14643 group showed improvement in intestinal mucosal damage and reduced infiltration of inflammatory cells. The protein expression of ZO-1 and occludin in colon of mice in the HFD+DSS+WY14643 was increased (all P＜0.05), while the expression of TNF-α, IL-1 β, and IL-17 mRNA was downregulated (P＜0.01 or P＜0.05), and the protein expression of PPAR α was upregulated(P＜0.05). Conclusions HFD-induced obesity aggravates intestinal mucosal damage, intestinal barrier destruction and inflammatory response in IBS mice, and its molecular mechanism is potentially related to downregulation of PPARα expression in intestinal tissues.

Key words: irritable bowel syndrome, obesity, peroxisome proliferator-activated receptor-α, intestinal barrier damage, inflammatory factors

中图分类号:

R365

赵翠娟, 敖民, 武文博, 李妍华. 高脂饮食加重小鼠肠易激综合征肠屏障损伤[J]. 基础医学与临床, 2025, 45(8): 1022-1027.

ZHAO Cuijuan, AO Min, WU Wenbo, LI Yanhua. High fat diet aggravates intestinal barrier damage in mice with irritable bowel syndrome[J]. Basic & Clinical Medicine, 2025, 45(8): 1022-1027.

参考文献

[1] Lou TW, Yang RX, Fan JG. The global burden of fatty liver disease: the major impact of China[J].Hepatobiliary Surg Nutr,2024,13:119-123.
[2] 中华华医学会消化病学分会胃肠功能性疾病协作组与中华医学会消化病学分会胃肠动力学组, 2020年中国肠易激综合征专家共识意见[J]. 中华消化杂志, 2020. 40: 803-818.
[3] Linsalata M, Riezzo G, Orlando A, et al. The role of intestinal barrier function in overweight patients with IBS with diarrhea undergoing a long-term low fermentable oligo-, Di-, and Monosaccharide and Polyol Diet[J].Nutrients,2023,15:4683.doi: 10.1186/s40360-018-0279-1.
[4] Ng JJJ, Loo WM, Siah KTH. Associations between irritable bowel syndrome and non-alcoholic fatty liver disease: A systematic review[J]. World J Hepatol,2023,15:925-938.
[5] Qiu YY, Zhang J, Zeng FY,et al. Roles of the peroxisome proliferator-activated receptors (PPARs) in the pathogenesis of nonalcoholic fatty liver disease (NAFLD)[J]. Pharmacol Res,2023,192: 106786.
[6] Grabacka M, Płonka PM, Pierzchalska M. The PPARα regulation of the gut physiology in regard to interaction with microbiota, intestinal immunity, metabolism, and permeability[J].Int J Mol Sci, 2022, 23:14156. doi: 10.3390/ijms232214156
[7] Oka P, Parr H, Barberio B, et al. Global prevalence of irritable bowel syndrome according to Rome Ⅲ or Ⅳ criteria: a systematic review and meta-analysis[J]. Lancet Gastroenterol Hepatol, 2020,5: 908-917.
[8] Hung TH, Wang CY, Lee HF. Update in diagnosis and management of irritable bowel syndrome[J]. Tzu Chi Med J, 2023,35:306-311.
[9] Black CJ, Staudacher HM, Ford AC. Efficacy of a low FODMAP diet in irritable bowel syndrome: systematic review and network meta-analysis[J]. Gut, 2022,71:1117-1126.
[10] Inczefi O, Bacsur P, Resál T, et al. The influence of nutrition on intestinal permeability and the microbiome in health and disease[J]. Front Nutr, 2022,9:718710.doi:10.3389/fnut.2022.718710.
[11] Xin D, Zong-Shun L, Bang-Mao W, et al. Expression of intestinal tight junction proteins in patients with non-alcoholic fatty liver disease[J]. Hepatogastroenterology, 2014, 61:136-140.
[12] Quesada-Vazquez S, Bone C, Saha S, et al. Microbiota dysbiosis and gut barrier dysfunction associated with non-alcoholic fatty liver disease are modulated by a specific metabolic cofactors' combination[J]. Int J Mol Sci,2022,23:23.doi: 10.3390/ijms232213675.
[13] Berthier A, Johanns M, Zummo FP, et al. PPARs in liver physiology[J]. Biochim Biophys Acta Mol Basis Dis, 2021,1867:166097.doi:10.3390/ijms232213675.
[14] Decara J, Rivera P, López-Gambero AJ, et al.Peroxisome proliferator-activated receptors: experimental targeting for the treatment of inflammatory bowel diseases[J]. Front Pharmacol, 2020,11:730.doi:10.3389/fphar.2020.00730.
[15] Pinna G. Role of PPAR-allopregnanolone signaling in behavioral and inflammatory gut-brain axis communications[J]. Biol Psychiatry,2023,94:609-618.
[16] Zuo J, Ding Q, He S,et al. Hepatic cytochrome P450 8B1 and cholic acid potentiate intestinal epithelial injury in colitis by suppressing intestinal stem cell renewal[J]. Cell Stem Cell, 2022,29:1366-1381.

高脂饮食加重小鼠肠易激综合征肠屏障损伤

High fat diet aggravates intestinal barrier damage in mice with irritable bowel syndrome

PDF

可视化

摘要/Abstract

引用本文

使用本文

参考文献

相关文章 15

编辑推荐

Metrics

本文评价

[1]	向韵瑄, 常晓悦. 肥胖促进哮喘发作的研究进展[J]. 基础医学与临床, 2025, 45(8): 1103-1107.
[2]	路少崇, 叶浩桢, 侯宋媛, 周业胜, 刘思, 朱圣韬. 肠道代谢物同型半胱氨酸参与调节肠易激综合征[J]. 基础医学与临床, 2025, 45(7): 858-865.
[3]	阿比旦·阿卜杜如苏力, 陈小翠, 崔元峰, 托罗娜依·米吉提, 邓李惠, 陈邦党. 人源PCSK9^D374Y加重蛋氨酸胆碱缺乏饮食诱导的小鼠非酒精性脂肪性肝炎[J]. 基础医学与临床, 2025, 45(5): 637-643.
[4]	胡艳敏, 彭丽娜, 杨勇, 向韵瑄, 常晓悦. Pleckstrin同源域家族A成员1在代谢性疾病中的作用[J]. 基础医学与临床, 2025, 45(2): 268-272.
[5]	加孜热亚·再依拿提, 李素丽, 张凯迪, 马福慧, 马国英, 郭艳英. 桥本甲状腺炎中辅助T细胞及其细胞因子与腹型肥胖相关[J]. 基础医学与临床, 2024, 44(8): 1120-1125.
[6]	丁宝锋, 王小爽, 王芳, 余佳. 肥胖模型小鼠肝脏的病理变化及代谢组分析[J]. 基础医学与临床, 2024, 44(5): 699-704.
[7]	张沥元, 杜函泽, 潘慧. 治疗下丘脑性肥胖的药物研究进展[J]. 基础医学与临床, 2024, 44(5): 729-732.
[8]	卢慧莹, 王建国. 下调去甲基化酶FTO抑制人肝癌细胞系HepG2增殖[J]. 基础医学与临床, 2024, 44(2): 185-191.
[9]	廖镇城, 杨思懿, 吴平安. 提高m⁶A去甲基化酶FTO表达抑制鼻咽癌细胞增殖[J]. 基础医学与临床, 2024, 44(1): 57-62.
[10]	马国英, 加孜热亚·再依拿提, 李素丽, 郭艳英. 基于血清蛋白质组学分析桥本甲状腺炎合并肥胖患者血清蛋白质差异表达[J]. 基础医学与临床, 2023, 43(9): 1375-1382.
[11]	陈辛, 陈俊, 徐幸, 王旭. 组蛋白去甲基化酶抑制剂GSK-J4减轻高脂诱导的肥胖小鼠体质量[J]. 基础医学与临床, 2023, 43(9): 1353-1358.
[12]	王鑫瑞, 秦燕. Ghrelin在代谢性疾病中作用的研究进展[J]. 基础医学与临床, 2023, 43(8): 1299-1303.
[13]	张晶, 吴凯, 黄伟. 人前体脂肪细胞分化过程及肥胖人群脂肪组织中hsa_circ_0017650高表达[J]. 基础医学与临床, 2023, 43(7): 1079-1083.
[14]	蒋晨晨, 崔泽, 潘利, 孙纪新, 何慧婧, 胡耀达, 单广良. 河北省汉族和满族成人高血压家族史与超重/肥胖对高血压发病的交互作用[J]. 基础医学与临床, 2023, 43(7): 1053-1059.
[15]	李晓娜, 齐先梅, 张田甜, 王婧. 沉默Fcgr3降低SiO₂诱导的小鼠肺泡巨噬细胞系MH-S炎性因子表达[J]. 基础医学与临床, 2023, 43(6): 904-908.