脑死亡期间肠道菌群失调和肝脏代谢组学变化

Ruolin Tao , Wenzhi Guo , Tao Li , Yong Wang , Panliang Wang
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引用次数: 0

摘要

背景脑死亡(BD)与肠道微生物群失调之间是否存在因果关系尚不清楚,与BD相关的肝脏代谢扭曲需要进一步探索。方法建立BD大鼠模型,持续9h(BD组,n=6)。假手术组(n=6)接受了相同的手术,但导管插入硬膜外腔而没有膨胀。收集肠道内容物和门静脉血浆进行微生物群测序和微生物代谢产物检测。切除肝组织以研究代谢变化,并将结果与假手术组的结果进行比较。结果α-多样性指数表明BD不改变细菌多样性。BD组9小时后出现微生物群失调。在家族水平上,BD组中的Peptostrectococcaceae和Bacteroidaceae均减少。在属水平上,Romboutsia、拟杆菌属、丹皮菌属_UG_004、Faecalibacterium和Barnesiella在假手术组中富集,而Ruminococcaceae _UG_007、Lachnospiraceae _ND3007_group和巴氏杆菌属在BD组中富集。BD组的肠道内容物和门静脉血浆中的短链脂肪酸、胆汁酸和132种其他微生物代谢产物保持不变。BD引起肝脏65种代谢产物的改变,其中碳水化合物、氨基酸和有机酸占64.6%。此外,BD组肝脏中80.0%的差异代谢产物减少。半乳糖代谢是BD组最重要的代谢途径。结论sBD可导致大鼠微生物群失调;然而,这种微生态失调并没有改变微生物的代谢产物。长期BD期间肝脏代谢功能的恶化可能反映了能量缺乏的持续恶化。
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Intestinal microbiota dysbiosis and liver metabolomic changes during brain death

Background

Whether a causative link exists between brain death (BD) and intestinal microbiota dysbiosis is unclear, and the distortion in liver metabolism associated with BD requires further exploration.

Methods

A rat model of BD was constructed and sustained for 9 h (BD group, n=6). The sham group (n=6) underwent the same procedures, but the catheter was inserted into the epidural space without ballooning. Intestinal contents and portal vein plasma were collected for microbiota sequencing and microbial metabolite detection. Liver tissue was resected to investigate metabolic alterations, and the results were compared with those of a sham group.

Results

α-diversity indexes showed that BD did not alter bacterial diversity. Microbiota dysbiosis occurred after 9 h of BD. At the family level, Peptostreptococcaceae and Bacteroidaceae were both decreased in the BD group. At the genus level, Romboutsia, Bacteroides, Erysipelotrichaceae_UCG_004, Faecalibacterium, and Barnesiella were enriched in the sham group, whereas Ruminococcaceae_UCG_007, Lachnospiraceae_ND3007_group, and Papillibacter were enriched in the BD group. Short-chain fatty acids, bile acids, and 132 other microbial metabolites remained unchanged in both the intestinal contents and portal vein plasma of the BD group. BD caused alterations in 65 metabolites in the liver, of which, carbohydrates, amino acids, and organic acids accounted for 64.6%. Additionally, 80.0% of the differential metabolites were decreased in the BD group livers. Galactose metabolism was the most significant metabolic pathway in the BD group.

Conclusions

BD resulted in microbiota dysbiosis in rats; however, this dysbiosis did not alter microbial metabolites. Deterioration in liver metabolic function during extended periods of BD may reflect a continuous worsening in energy deficiency.

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来源期刊
Journal of intensive medicine
Journal of intensive medicine Critical Care and Intensive Care Medicine
CiteScore
1.90
自引率
0.00%
发文量
0
审稿时长
58 days
期刊最新文献
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