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蔓越莓多酚和龙舌兰低聚果糖可影响肠道免疫反应和微生物组成,同时改善喂食致肥胖饮食的小鼠的肠道屏障功能、炎症和葡萄糖代谢。

Cranberry polyphenols and agave agavins impact gut immune response and microbiota composition while improving gut barrier function, inflammation, and glucose metabolism in mice fed an obesogenic diet.

机构信息

Institute of Nutrition and Functional Foods (INAF), Laval University, Québec, QC, Canada.

School of Nutrition, Faculty of Agriculture and Food Sciences, Laval University, Québec, QC, Canada.

出版信息

Front Immunol. 2022 Aug 16;13:871080. doi: 10.3389/fimmu.2022.871080. eCollection 2022.

Abstract

The consumption of plant-based bioactive compounds modulates the gut microbiota and interacts with the innate and adaptive immune responses associated with metabolic disorders. The present study aimed to evaluate the effect of cranberry polyphenols (CP), rich in flavonoids, and agavins (AG), a highly branched agave-derived neo-fructans, on cardiometabolic response, gut microbiota composition, metabolic endotoxemia, and mucosal immunomodulation of C57BL6 male mice fed an obesogenic high-fat and high-sucrose (HFHS) diet for 9 weeks. Interestingly, CP+AG-fed mice had improved glucose homeostasis. Oral supplementation with CP selectively and robustly (five-fold) increases the relative abundance of , a beneficial bacteria associated with metabolic health. AG, either alone or combined with CP (CP+AG), mainly stimulated the glycan-degrading bacteria , , , and This increase of glycan-degrading bacteria was consistent with a significantly increased level of butyrate in obese mice receiving AG, as compared to untreated counterparts. CP+AG-supplemented HFHS-fed mice had significantly lower levels of plasma LBP than HFHS-fed controls, suggesting blunted metabolic endotoxemia and improved intestinal barrier function. Gut microbiota and derived metabolites interact with the immunological factors to improve intestinal epithelium barrier function. Oral administration of CP and AG to obese mice contributed to dampen the pro-inflammatory immune response through different signaling pathways. CP and AG, alone or combined, increased toll-like receptor (TLR)-2 () expression, while decreasing the expression of interleukin 1ß (ILß1) in obese mice. Moreover, AG selectively promoted the anti-inflammatory marker , while CP increased the expression of NOD-like receptor family pyrin domain containing 6 () inflammasome. The intestinal immune system was also shaped by dietary factor recognition. Indeed, the combination of CP+AG significantly increased the expression of aryl hydrocarbon receptors (). Altogether, both CP and AG can shape gut microbiota composition and regulate key mucosal markers involved in the repair of epithelial barrier integrity, thereby attenuating obesity-associated gut dysbiosis and metabolic inflammation and improving glucose homeostasis.

摘要

植物源生物活性化合物的消耗会调节肠道微生物群,并与与代谢紊乱相关的先天和适应性免疫反应相互作用。本研究旨在评估富含类黄酮的蔓越莓多酚(CP)和甘露糖(AG)(一种高度分支的龙舌兰衍生的新果聚糖)对 9 周喂食致肥胖高糖高脂(HFHS)饮食的 C57BL6 雄性小鼠的心脏代谢反应、肠道微生物群组成、代谢内毒素血症和黏膜免疫调节的影响。有趣的是,CP+AG 喂养的小鼠改善了葡萄糖稳态。CP 的口服补充选择性且强烈(五倍)增加了有益细菌的相对丰度,该细菌与代谢健康相关。AG 无论是单独使用还是与 CP 联合使用(CP+AG),主要刺激聚糖降解细菌、、、和 。这种聚糖降解细菌的增加与肥胖小鼠中丁酸盐水平的显著增加一致,与未处理的对照相比,接受 AG 的肥胖小鼠的丁酸盐水平显著增加。与 HFHS 喂养的对照组相比,CP+AG 补充 HFHS 喂养的小鼠的血浆 LBP 水平显著降低,表明代谢内毒素血症减弱,肠道屏障功能改善。肠道微生物群及其衍生代谢物与免疫因素相互作用,改善肠道上皮屏障功能。CP 和 AG 的口服给予肥胖小鼠有助于通过不同的信号通路抑制促炎免疫反应。CP 和 AG 单独或联合使用可增加 Toll 样受体(TLR)-2()的表达,同时降低肥胖小鼠中白细胞介素 1β(IL1β)的表达。此外,AG 选择性促进抗炎标志物,而 CP 增加 NOD 样受体家族 pyrin 域包含 6()炎性小体的表达。肠道免疫系统也受到饮食因素识别的影响。事实上,CP+AG 的组合显著增加了芳香烃受体()的表达。总之,CP 和 AG 都可以改变肠道微生物群的组成,并调节与修复上皮屏障完整性相关的关键黏膜标志物,从而减轻肥胖相关的肠道菌群失调和代谢炎症,改善葡萄糖稳态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e7a0/9424773/4487722923f1/fimmu-13-871080-g001.jpg

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