番泻叶乙醇提取物(EESL)对小鼠炎症和氧化应激的影响:非靶向代谢组学研究。

Xiaoli Huang, Wen Sun, Chang Sun, Jiajun Tan, Liang Wu, Fumeng Yang
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引用次数: 0

摘要

背景:番泻叶是治疗便秘的常用药物,长期服用会对肠道黏膜造成损伤,并导致药物依赖。但其确切机制仍不清楚:利用非靶向代谢组学技术研究番泻叶乙醇提取物(EESL)诱导小鼠炎症和氧化应激反应并产生副作用的机制:结果:在番泻叶乙醇提取物中发现了23种蒽醌类化合物,包括番泻苷及其衍生物。给小鼠服用伊索苷后,血浆中的促炎因子、IL-1β和IL-6显著增加,而IgA水平显著下降。氧化应激水平明显升高,肠粘膜完整性受损。经鉴定,血浆中的 21 种内源性代谢物与牛磺酸和牛磺酸代谢、甘油磷脂代谢、花生四烯酸代谢、色氨酸代谢和鞘脂代谢有关。这些代谢途径与氧化应激和炎症有关:结论:番泻叶可抑制肠粘膜紧密连接蛋白的表达,破坏肠粘膜屏障的完整性,加剧氧化应激和细菌 LPS 进入血液后诱发的炎症。此外,番泻叶对色氨酸代谢的影响可能与药物依赖的发生有关。
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Effects of ethanol extract from senna leaf (EESL) on inflammation and oxidative stress in mice: A non-targeted metabolomic study.

Background: Senna leaf is a commonly used medication for treating constipation, and long-term use can cause damage to the intestinal mucosa and lead to drug dependence. But the exact mechanism remains unclear.

Objective: Using non-targeted metabolomics technology to study the mechanism of senna leaf ethanol extract (EESL) inducing inflammation and oxidative stress in mice and causing side effects.

Methods: EESL was administered to mice by gavage to detect inflammation and oxidative stressrelated factors in mice, and the EESL components and differential metabolites in mouse plasma were analyzed using non-targeted metabolome techniques.

Results: 23 anthraquinone compounds were identified in the EESL, including sennoside and their derivatives. Administration of EESL to mice resulted in a significant increase in pro-inflammatory factors, IL-1β, and IL-6 in the plasma, while the levels of IgA significantly decreased. The levels of oxidative stress significantly increased, and the intestinal mucosal integrity was impaired. 21 endogenous in plasma metabolites were identified as differential metabolites related with taurine and taurine metabolism, glycerophospholipid metabolism, arachidonic acid metabolism, tryptophan metabolism, and sphingolipid metabolism. These metabolic pathways are related to oxidative stress and inflammation.

Conclusion: Senna leaf can inhibit the expression of tight junction proteins in the intestinal mucosa and disrupt intestinal mucosal barrier integrity, exacerbating oxidative stress and inflammation induced by bacterial LPS entering the bloodstream. In addition, the impact of Senna leaf on tryptophan metabolism may be linked to the occurrence of drug dependence.

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