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Transformation of Psoralen and Isopsoralen by Human Intestinal Microbial In Vitro and the Biological Activities of Its Metabolites

机译:人体肠道微生物对补骨脂素和异补骨脂素的转化及其代谢产物的生物学活性

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摘要

Psoralen (P) and isopsoralen (IP) are the main active ingredients in the dried fruit of L. (PC), with a wide range of pharmacology activities. The intestinal bacteria biotransformation plays a central role in the metabolism of the complex ingredients in traditional Chinese medicine (TCM). Our study aimed to investigated the metabolic profile of P and IP in the intestinal condition, co-cultured with human fecal bacteria anaerobically. Four bio-transforming products were obtained, including 6,7-furano-hydrocoumaric acid (P-1) and 6,7-furano-hydro- coumaric acid methyl ester (P-2), which transformed from P, and 5,6-furano-hydrocoumaric acid (IP-1) and 5,6-furano-hydrocoumaric acid methyl ester (IP-2), which were transformed from IP. It is worth mentioning that IP-2 is a new compound that has not been published. Their structures were analyzed based on their spectroscopic data. Moreover, a highly sensitive ultra-performance liquid chromatography tandem mass spectrometry (UPLC-MS/MS) method was used to characterize the metabolic pathways of P, IP, and their bio-transforming products in the reaction samples. In addition, the dampening effects against the oxidative stress of P, IP, and their bio-transforming products by human intestinal flora were estimated in vitro via the human colorectal cells (HCT116) and heterogeneous human epithelial colorectal adenocarcinoma cells (Caco-2) cell lines. The results showed that the metabolites have stronger activity than P and IP, which possibly provides a basis for elucidating the treating mechanisms of PC extract against inflammatory bowel disease.
机译:补骨脂素(P)和异补骨脂素(IP)是L.(PC)干果中的主要活性成分,具有广泛的药理活性。肠道细菌的生物转化在中药(TCM)中复杂成分的代谢中起着核心作用。我们的研究旨在调查在肠道条件下与人类粪便细菌厌氧共培养的P和IP的代谢特征。获得了四种生物转化产物,包括从P转化而来的6,7-呋喃-氢香豆酸(P-1)和6,7-呋喃-氢香豆酸甲酯(P-2)和5,6 -从IP转化的-呋喃-氢香豆酸(IP-1)和5,6-呋喃-氢香豆酸甲酯(IP-2)。值得一提的是IP-2是尚未发布的新化合物。根据其光谱数据分析其结构。此外,使用高灵敏度超高效液相色谱串联质谱法(UPLC-MS / MS)表征反应样品中P,IP及其生物转化产物的代谢途径。此外,还通过人结肠直肠细胞(HCT116)和异种人上皮结肠直肠腺癌细胞(Caco-2)细胞体外评估了人肠道菌群对P,IP及其生物转化产物的氧化应激的抑制作用。线。结果表明,该代谢产物的活性高于P和IP,这可能为阐明PC提取物抗炎性肠病的机制提供了依据。

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