武平紫芝β-葡聚糖对急性酒精性肝损伤小鼠肠道菌群及其代谢的作用机制

doi:10.7506/spkx1002-6630-20241101-004

摘要/Abstract

摘要： 以武平紫芝的活性单糖β-葡聚糖为研究对象，通过肠道菌群及其代谢物的关联研究探讨灵芝多糖对急性酒精性肝损伤小鼠肝脏的保护作用机制。将180 只清洁级小鼠随机分为6 组，包括空白组（水空白组、羧甲基纤维素钠空白组）、模型组（水模型组、羧甲基纤维素钠模型组）、实验组（200 mg/kg紫芝β-葡聚糖）和阳性对照组（300 mg/kg联苯双酯）。连续灌胃处理一周后，检测各组的血清、肝组织的生化指标及肝脏病理切片，并分析小鼠肠道菌群的及代谢产物组成的差异。结果表明，灌胃200 mg/kg紫芝β-葡聚糖可改善急性酒精性肝损伤小鼠的肝功能，与模型组小鼠相比，紫芝β-葡聚糖实验组的丙氨酸氨基转移酶、甘油三酯、总胆固醇、丙二醛、乙醇脱氢酶水平显著降低（P＜0.05），总超氧化物歧化酶、还原型谷胱甘肽水平显著增高（P＜0.05）。小鼠肝脏病理学分析证实，紫芝β-葡聚糖可显著改善肝细胞、肝小叶病变，对肝脏保护起到了一定的作用。紫芝β-葡聚糖改善了小鼠的肠道菌群及物质代谢，具体表现为，与模型组相比，紫芝β-葡聚糖实验组Firmicutes/Bacteroidota比值升高，Firmicutes的GCA-900066575、Roseburia等有益菌群相对丰度明显升高，Bacteroidota的Bacteroides使得胆固醇、DHA乙酯、油酸甲酯等脂类及类脂分子及Firmicutes的Lactobacillus使得丙酸等物质代谢的改变从而改善了小鼠急性酒精性肝损伤。因此，灵芝多糖对急性酒精性肝损伤小鼠肝脏的保护作用机制可能是通过改善动物肠道菌群组成调节氨基酸代谢、脂类及类脂分子代谢和丙酸代谢，从而发挥保肝护肝作用。

关键词: 武平紫芝；β-葡聚糖；急性酒精性肝损伤；肠道菌群；肠道代谢物；保肝作用

Abstract: This study shed light on the hepatoprotective mechanism of β-glucan from Ganoderma sinense produced in Wuping, China on mice with acute alcoholic liver injury (AALI) through studies on the correlation between the gut microbiota and its metabolites. A total of 180 specific pathogen-free (SPF)-grade mice were randomly assigned to six groups: two control groups (CK and A, gavaged with distilled water and carboxymethyl cellulose sodium (CMC-Na), respectively), two model groups (C and D, gavaged with distilled water and CMC-Na, respectively), an experimental group (D, gavaged with 200 mg/kg of G. lucidum β-glucan), and a positive control group (E, gavaged with 300 mg/kg of diphenyl diester). After one week of continuous administration, serum and liver biochemical indices were measured in each group and histopathological observation of liver sections was studied. Meanwhile, the differences in the composition of the intestinal microbiota and metabolites were analyzed among groups. The results indicated that oral administration of 200 mg/kg of G. sinense β-glucan ameliorated liver function in AALI mice. Compared with the model groups, the experimental group exhibited significantly reduced levels of alanine aminotransferase (ALT), triglyceride (TG), total cholesterol (TC), malondialdehyde (MDA) and alcohol dehydrogenase (ADH) (P < 0.05) and significantly increased levels of total superoxide dismutase (T-SOD) and reduced glutathione (GSH) (P < 0.05). Histopathological observation confirmed that β-glucan from G. lucidum significantly attenuated liver cell and lobular lesions, thereby exerting a hepatoprotective effect. G. sinense β-glucan improved the gut microbiota and substance metabolism in mice. Specifically, compared with the model group, the ratio of Firmicutes/Bacteroidoota (F/B) increased in the experimental group, and the relative abundance of beneficial bacteria such as GCA-900066575 and Roseburia in Firmicutes significantly increased as well. Additionally, G. sinense β-glucan altered the metabolism of lipids and lipid-like molecules such as cholesterol, DHA ethyl ester, and oleic acid methyl ester through affecting Bacteroides in the Bacteroidota phylum and altered propionic acid metabolism through affecting Lactobacillus in the Firmicutes phylum, thereby alleviating AALI. Therefore, the protective mechanism of G. sinense polysaccharides against AALI in mice might be related to the regulation of amino acid metabolism, lipid and lipid-like molecule metabolism, and propionic acid metabolism by improving the composition of the gut microbiota.

Key words: Ganoderma sinense from Wuping; β-glucan; acute alcoholic liver injury; gut microbiota; intestinal metabolites; hepatoprotective effect

中图分类号:

R151.2

林标声，王金平，王武昌，陈彤，林炜明，沈绍新. 武平紫芝β-葡聚糖对急性酒精性肝损伤小鼠肠道菌群及其代谢的作用机制[J]. 食品科学, 2025, 46(13): 185-155.

LIN Biaosheng, WANG Jinping, WANG Wuchang, CHEN Tong, Lin Weiming, SHEN Shaoxin. Action Mechanism of β-Glucan from Ganoderma sinense Produced in Wuping on Gut Microbiota and Metabolism in Mice with Acute Alcoholic Liver Injury[J]. FOOD SCIENCE, 2025, 46(13): 185-155.

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武平紫芝β-葡聚糖对急性酒精性肝损伤小鼠肠道菌群及其代谢的作用机制

Action Mechanism of β-Glucan from Ganoderma sinense Produced in Wuping on Gut Microbiota and Metabolism in Mice with Acute Alcoholic Liver Injury

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