肠道微生物群介导了对乙酰氨基酚诱导的小鼠急性肝损伤的昼夜变化。
Gut microbiota mediates diurnal variation of acetaminophen induced acute liver injury in mice.
机构信息
State Key Laboratory of Organ Failure Research, Southern Medical University, Guangzhou, China; Guangdong Provincial Key Laboratory of Proteomics, Southern Medical University, Guangzhou, China; Department of Pathophysiology, Southern Medical University, Guangzhou, China.
Guangdong Pharmaceutical University, Guangzhou, China.
出版信息
J Hepatol. 2018 Jul;69(1):51-59. doi: 10.1016/j.jhep.2018.02.024. Epub 2018 Mar 8.
BACKGROUND & AIMS: Acetaminophen (APAP) induced hepatotoxicity is a leading cause of acute liver failure worldwide. It is well established that the liver damage induced by acetaminophen exhibits diurnal variation. However, the detailed mechanism for the hepatotoxic variation is not clear. Herein, we aimed to determine the relative contributions of gut microbiota in modulating the diurnal variation of hepatotoxicity induced by APAP.
METHODS
Male Balb/C mice were treated with or without antibiotics and a single dose of orally administered APAP (300 mg/kg) at ZT0 (when the light is on-start of resting period) and ZT12 (when the light is off-start of active period).
RESULTS
In agreement with previous findings, hepatic injury was markedly enhanced at ZT12 compared with ZT0. Interestingly, upon antibiotic treatment, ZT12 displayed a protective effect against APAP hepatotoxicity similar to ZT0. Moreover, mice that received the cecal content from ZT12 showed more severe liver damage than mice that received the cecal content from ZT0. 16S sequencing data revealed significant differences in the cecal content between ZT0 and ZT12 in the compositional level. Furthermore, metabolomic analysis showed that the gut microbial metabolites were also different between ZT0 and ZT12. Specifically, the level of 1-phenyl-1,2-propanedione (PPD) was significantly higher at ZT12 than ZT0. Treatment with PPD alone did not cause obvious liver damage. However, PPD synergistically enhanced APAP-induced hepatic injury in vivo and in vitro. Finally, we found Saccharomyces cerevisiae, which could reduce intestinal PPD levels, was able to markedly alleviate APAP-induced liver damage at ZT12.
CONCLUSIONS
The gut microbial metabolite PPD was responsible, at least in part, for the diurnal variation of hepatotoxicity induced by APAP by decreasing glutathione levels.
LAY SUMMARY
Acetaminophen (APAP) induced acute liver failure because of over dose is a leading public health problem. APAP-induced liver injury exhibits diurnal variation, specifically APAP causes more severe liver damage when taken at night compared with in the morning. Herein, we showed that gut microbial metabolite, 1-phenyl-1,2-propanedione is involved in the rhythmic hepatotoxicity induced by APAP, by depleting hepatic glutathione (an important antioxidant) levels. Our data suggest gut microbiota may be a potential target for reducing APAP-induced acute liver injury.
背景与目的
醋氨酚(APAP)诱导的肝毒性是全球急性肝衰竭的主要原因。众所周知,醋氨酚引起的肝损伤具有昼夜变化。然而,肝毒性变化的详细机制尚不清楚。在此,我们旨在确定肠道微生物群在调节 APAP 诱导的肝毒性昼夜变化中的相对贡献。
方法
雄性 Balb/C 小鼠接受或不接受抗生素治疗,并在 ZT0(光照开始休息期)和 ZT12(光照关闭活动期)时给予单次口服 APAP(300mg/kg)。
结果
与先前的发现一致,与 ZT0 相比,ZT12 时肝损伤明显加重。有趣的是,接受抗生素治疗后,ZT12 对 APAP 肝毒性表现出与 ZT0 相似的保护作用。此外,接受 ZT12 盲肠内容物的小鼠比接受 ZT0 盲肠内容物的小鼠显示出更严重的肝损伤。16S 测序数据显示,ZT0 和 ZT12 之间的盲肠内容物在组成水平上存在显著差异。此外,代谢组学分析显示,ZT0 和 ZT12 之间的肠道微生物代谢物也不同。具体而言,ZT12 时 1-苯-1,2-丙二酮(PPD)水平明显高于 ZT0。单独使用 PPD 不会引起明显的肝损伤。然而,PPD 协同增强了体内和体外的 APAP 诱导的肝损伤。最后,我们发现可以降低肠道 PPD 水平的酿酒酵母(Saccharomyces cerevisiae)能够显著缓解 ZT12 时 APAP 诱导的肝损伤。
结论
肠道微生物代谢物 PPD 通过降低谷胱甘肽水平,至少部分负责 APAP 诱导的肝毒性的昼夜变化。
简要说明
过量服用醋氨酚(APAP)引起的急性肝衰竭是一个主要的公共卫生问题。APAP 诱导的肝损伤具有昼夜变化,具体来说,与早上相比,晚上服用 APAP 会导致更严重的肝损伤。在此,我们表明肠道微生物代谢物 1-苯-1,2-丙二酮(1-phenyl-1,2-propanedione,PPD)通过消耗肝内谷胱甘肽(一种重要的抗氧化剂)水平,参与 APAP 诱导的节律性肝毒性。我们的数据表明,肠道微生物群可能是减少 APAP 诱导的急性肝损伤的潜在靶点。
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