Protective mechanisms of Tuina therapy against lipopolysaccharide-induced fever in young rabbits based on untargeted metabolomics analysis.

Liu Di, Zhang Yingqi, Y U Tianyuan, Liu Zhifeng, Jiao Yi, Wang Hourong, X U Yajing, Guan Qian, Chen Lulu, H U Hui
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Abstract

Objective: To investigate the effect of Tuina on the plasma metabolites of lipopolysaccharide-induced febrile in infant rabbits.

Methods: Twenty-four infant New Zealand rabbits were selected and randomly divided into three groups: saline, model, and Tuina. The fever model was established by injecting LPS intravenously through the ear margin vein in the model group and Tuina group, respectively. The modeling was considered successful when the anal temperature increased by 0.5℃ or above within 1 h. In the Tuina group, six Tuina techniques (i.e., opening Tianmen / the heaven gate, pushing Kangong / the superciliary arch, kneading Taiyang and the prominent bone behind the ears, clearing Tianheshui, spine pinching) that alleviate fever were performed on the young rabbits 1 h after the modeling, whereas the model and saline groups were not given Tuina treatment, with the real-time anal temperature monitored during the experiment. The plasma was taken 3 h after the modeling for liquid chromatography-mass spectrometry (LC-MS) untargeted metabolomics study.

Results: Our results showed a fever-reducing effects of Tuina therapy on lipopolysaccharide-induced fever in young rabbits, as indicated by a significantly lower anal temperature, maximum rise in body temperature, and body response index at 2 and 3 h after modeling in the Tuina group compared to the model group, with reductions in the PGE2 expression observed in the blood and hypothalamus. The differential metabolites including riboflavin, nicotinamide N-oxide, porphobilinogen, 5-hydroxyindoleacetic acid, gamma-aminobutyric acid, and lysoPC (16:1 (9Z)/0:0) were found following the Tuina intervention. Tuina primarily involves glycine-serine-threonine, arginine-proline, porphyrin-chlorophyll, pyrimidine, primary bile acid biosynthesis, and cyanoamino acid metabolic pathways.

Conclusion: Tuina therapy has proven to be effective in reducing body temperature and down-regulating PGE2 expression in LPS-induced febrile young rabbits, with its mechanism of fever-reducing action possibly associated with the changes in plasma metabolites and metabolic pathways.

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基于非靶向代谢组学分析的推拿疗法对脂多糖诱发幼兔发热的保护机制
目的研究推拿对脂多糖诱发幼兔发热血浆代谢物的影响:方法:选取 24 只新西兰幼兔,随机分为三组:生理盐水组、模型组和推拿组。模型组和 Tuina 组分别通过耳缘静脉注射 LPS 建立发热模型。模型组在 1 小时内肛温升高 0.5℃或以上为成功、模型组和生理盐水组不进行推拿治疗,实验过程中实时监测肛温。建模 3 小时后取血浆进行液相色谱-质谱(LC-MS)非靶向代谢组学研究:结果:我们的研究结果表明,推拿疗法对脂多糖诱导的幼兔发热有退热作用,表现为推拿组与模型组相比,模型后 2 和 3 h 的肛温、体温最高升幅和身体反应指数明显降低,同时在血液和下丘脑中观察到 PGE2 表达减少。在推拿干预后发现了不同的代谢物,包括核黄素、烟酰胺 N-氧化物、卟啉原、5-羟基吲哚乙酸、γ-氨基丁酸和溶菌酸(16:1 (9Z)/0:0)。推拿主要涉及甘氨酸-丝氨酸-苏氨酸、精氨酸-脯氨酸、卟啉-叶绿素、嘧啶、初级胆汁酸生物合成和氰基氨基酸代谢途径:事实证明,推拿疗法能有效降低 LPS 诱导的发热幼兔的体温并下调 PGE2 的表达,其退热作用机制可能与血浆代谢物和代谢途径的变化有关。
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