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后生元通过保护细胞免受氧化损伤、改善脂质代谢和调节肠道微生物群来改善急性酒精性肝损伤。

-Derived Postbiotics Ameliorate Acute Alcohol-Induced Liver Injury by Protecting Cells from Oxidative Damage, Improving Lipid Metabolism, and Regulating Intestinal Microbiota.

机构信息

School of Laboratory Medicine and Life Science, Wenzhou Medical University, Wenzhou 325035, China.

Healthcare Center of the First Affiliated Hospital of Wenzhou Medical University, Wenzhou 325000, China.

出版信息

Nutrients. 2023 Feb 7;15(4):845. doi: 10.3390/nu15040845.

Abstract

Here, the aim was to evaluate the protective effect of -derived postbiotics, i.e., LP-cs, on acute alcoholic liver injury (ALI). After preincubation with LP-cs, HL7702 human hepatocytes were treated with alcohol, and then the cell survival rate was measured. C57BL/6 male mice were presupplemented with or without LP-cs and LP-cs-loaded calcium alginate hydrogel (LP-cs-Gel) for 3 weeks and given 50% alcohol gavage to establish the mouse model of ALI, LP-cs presupplementation, and LP-cs-Gel presupplementation. The histomorphology of the liver and intestines; the levels of serum AST, ALT, lipid, and SOD activity; liver transcriptomics; and the metagenome of intestinal microbiota were detected in all mouse models. In vitro, LP-cs significantly increased the survival rate of alcohol-treated cells. In vivo, presupplementation with LP-cs and LP-cs-Gel restored the levels of serum AST, ALT, and SOD activity, as well as TC and TG, after acute alcohol intake. In the LP-cs-presupplemented mice, the genes involved in fatty acid metabolic processes were upregulated and the genes involved in steroid biosynthesis were downregulated significantly as compared with the ALI mice. LP-cs significantly increased the abundance of intestinal microbiota, especially . In conclusion, LP-cs ameliorates ALI by protecting hepatocytes against oxidative damage, thereby, improving lipid metabolism and regulating the intestinal microbiota. The effect of LP-cs-Gel is similar to that of LP-cs.

摘要

在这里,目的是评估源自 LP 的后生元,即 LP-cs,对急性酒精性肝损伤 (ALI) 的保护作用。在用 LP-cs 孵育后,HL7702 人肝细胞用酒精处理,然后测量细胞存活率。C57BL/6 雄性小鼠用或不用 LP-cs 和负载 LP-cs 的海藻酸钠水凝胶 (LP-cs-Gel) 预先补充 3 周,并给予 50%酒精灌胃,建立 ALI 小鼠模型、LP-cs 预先补充和 LP-cs-Gel 预先补充。检测所有小鼠模型的肝和肠组织形态学;血清 AST、ALT、脂质和 SOD 活性水平;肝转录组学;和肠道微生物组的宏基因组。体外,LP-cs 显著提高了酒精处理细胞的存活率。在体内,LP-cs 和 LP-cs-Gel 的预先补充在急性酒精摄入后恢复了血清 AST、ALT 和 SOD 活性以及 TC 和 TG 的水平。在 LP-cs 补充的小鼠中,与 ALI 小鼠相比,参与脂肪酸代谢过程的基因上调,参与类固醇生物合成的基因下调显著。LP-cs 显著增加了肠道微生物群的丰度,特别是 。总之,LP-cs 通过保护肝细胞免受氧化损伤来改善 ALI,从而改善脂质代谢并调节肠道微生物群。LP-cs-Gel 的效果与 LP-cs 相似。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/78ab/9965849/79bd4bdecc2a/nutrients-15-00845-g001.jpg

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