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Effect of artesunate supplementation on bacterial translocation and dysbiosis of gut microbiota in rats with liver cirrhosis

机译:青蒿琥酯对肝硬化大鼠肠道菌群细菌移位和代谢障碍的影响。

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摘要

AIM: To evaluate the effect of artesunate (AS) supplementation on bacterial translocation (BT) and gut microbiota in a rat model of liver cirrhosis.METHODS: Fifty-four male Sprague-Dawley rats were randomly divided into a normal control group (N), a liver cirrhosis group (M) and a liver cirrhosis group intervened with AS (MA). Each group was sampled at 4, 6 and 8 wk. Liver cirrhosis was induced by injection of carbon tetrachloride (CCl4), intragastric administration of 10% ethanol, and feeding a high fat diet. Rats in the MA group were intragastrically administered with AS (25 mg/kg body weight, once daily). Injuries of the liver and intestinal mucosa were assessed by hematoxylin-eosin or Masson’s trichrome staining. Liver index was calculated as a ratio of the organ weight (g) to body weight (g). The gut microbiota was examined by automated ribosomal intergenic-spacer analysis of fecal DNA. BT was assessed by standard microbiological techniques in the blood, mesenteric lymph nodes (MLNs), liver, spleen, and kidney.RESULTS: Compared to group N, the body weight was reduced significantly in groups M and MA due to the development of liver cirrhosis over the period of 8 wk. The body weight was higher in group MA than in group M. The liver indices were significantly elevated at 4, 6 and 8 wk in groups M and MA compared to group N. AS supplementation partially decreased the liver indices in group MA. Marked histopathologic changes in the liver and small intestinal mucosa in group M were observed, which were alleviated in group MA. Levels of pro-inflammatory interleukin-6 and tumor necrosis factor-α were significantly elevated at 8 wk in ileal homogenates in group M compared to group N, which were decreased after AS supplementation in group MA. The dysbiosis of gut microbiota indicated by the mean diversity (Shannon index) and mean similarity (Sorenson index) was severe as the liver cirrhosis developed, and AS supplementation had an apparent intervention effect on the dysbiosis of gut microbiota at 4 wk. The occurrence of BT was increased in the liver of group M compared to that of group N. AS supplementation reduced BT in group MA at 8 wk. BT also occurred in the MLNs, spleen, and kidney, which was reduced by AS supplementation. BT was not detected in the blood in any group.CONCLUSION: Dysbiosis of gut microbiota, injury of intestinal mucosal barrier and BT occurred as liver cirrhosis progressed, which might enhance inflammation and aggravate liver injury. AS may have other non-antimalarial effects that modulate gut microbiota, inhibit BT and alleviate inflammation, resulting in a reduction in CCl4, alcohol and high fat-caused damages to the liver and intestine.
机译:目的:评价青蒿琥酯(AS)对肝硬化大鼠模型细菌移位(BT)和肠道菌群的影响。方法:54只雄性Sprague-Dawley大鼠随机分为正常对照组(N)。 ,肝硬化组(M)和肝硬化组干预AS(MA)。每组分别在第4、6和8周取样。通过注射四氯化碳(CCl4),在胃内给予10%的乙醇并喂养高脂饮食来诱发肝硬化。 MA组的大鼠在胃内给予AS(25 mg / kg体重,每天一次)。用苏木精-伊红或马森三色染色评估肝脏和肠粘膜的损伤。以器官重量(g)与体重(g)之比计算肝脏指数。通过粪便DNA的核糖体基因间-间隔自动分析检查肠道菌群。通过标准微生物学技术对血液,肠系膜淋巴结(MLN),肝脏,脾脏和肾脏中的BT进行评估。结果:与N组相比,由于肝硬化的发展,M和MA组的体重显着降低在8周内。 MA组的体重高于M组。与N组相比,M组和MA在第4、6和8周的肝脏指数显着升高。补充AS可以部分降低MA组的肝脏指数。 M组观察到肝脏和小肠粘膜明显的组织病理学改变,而MA组则得到缓解。与N组相比,M组回肠匀浆中促炎性白细胞介素6和肿瘤坏死因子-α的水平在8周时显着升高,而在MA组中补充AS后降低。随着肝硬化的发展,以平均多样性(Shannon指数)和平均相似度(Sorenson指数)表示的肠道菌群失调严重,并且在4 wk时,AS补充对肠道菌群失调有明显的干预作用。与N组相比,M组的肝脏中BT的发生增加。AS补充在8周时降低了MA组的BT。 BT也出现在MLN,脾脏和肾脏中,通过补充AS可以减少BT。结论:随着肝硬化的发展,肠道菌群失调,肠粘膜屏障损伤和BT发生,可能加剧炎症反应,加重肝损伤。 AS可能还有其他非抗动物作用,可调节肠道菌群,抑制BT并减轻炎症,从而降低CCl4,酒精含量以及高脂肪引起的肝脏和肠道损伤。

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