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Isolation and Identification of Twelve Metabolites of Isocorynoxeine in Rat Urine and their Neuroprotective Activities in HT22 Cell Assay

机译:大鼠尿液中异辛卡因的十二种代谢产物的分离鉴定及其在HT22细胞中的神经保护活性

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摘要

Isocorynoxeine, one of the major alkaloids from Uncaria Hook, shows the effects of lowering blood pressure, vasodilatation, and protection against ischemia-induced neuronal damage. In this paper, the metabolism of isocorynoxeine was investigated in rats. Twelve metabolites and the parent drug were isolated by using solvent extraction and repeated chromatographic methods, and determined by spectroscopic methods including UV, MS, NMR, and CD experiments. Seven new compounds were identified as 11-hydroxyisocorynoxeine, 5-oxoisocorynoxeinic acid-22-O-β-D-glucuronide, 10-hydroxyisocorynoxeine, 17-O-demethyl-16,17-dihydro-5-oxoisocorynoxeine, 5-oxoisocorynoxeinic acid, 21-hydroxy-5-oxoisocorynoxeine, and oxireno[,]-5-oxoisocorynoxeine, together with six known compounds identified as isocorynoxeine, 18,19-dehydrocorynoxinic acid, 18,19-dehydrocorynoxinic acid B, corynoxeine, isocorynoxeine-N-oxide, and corynoxeine-N-oxide. Possible metabolic pathways of isocorynoxeine are proposed. Furthermore, the activity assay for the parent drug and some of its metabolites showed that isocorynoxeine exhibited a significant neuroprotective effect against glutamate-induced HT22 cell death at the maximum concentration. However, little or weak neuroprotective activities were observed for M-3, M-6, M-7, and M-10. Our present study is important to further understand their metabolic fate and disposition in humans.
机译:异辛卡因(Unocaria Hook)的主要生物碱之一,具有降低血压,舒张血管和防止缺血引起的神经元损伤的作用。在本文中,研究了大鼠体内异corynoxeine的代谢。通过溶剂萃取和重复色谱法分离出十二种代谢物和母体药物,并通过包括UV,MS,NMR和CD实验在内的光谱方法进行测定。鉴定了7种新化合物,分别为11-羟基异皮质炔氧酸,5-氧异皮质炔氧酸22-O-β-D-葡糖醛酸,10-羟基异皮质炔氧酸,17-O-去甲基-16,17-二氢-5-氧杂异炔氧辛酸,5-氧杂异炔氧辛酸, 21-羟基-5-氧代异corynoxeine和oxireno [,]-5-氧代异corynoxeine,连同六个已知的化合物被鉴定为异corynoxeine,18,19-dehydrocorynoxinic acid,18,19-dehydrocorynoxinic acid B,corynoxeine,isocorynoxeine-N-oxide,和Corynoxeine-N-氧化物。提出了异corynoxeine可能的代谢途径。此外,对母体药物及其某些代谢产物的活性测定表明,异高炔异辛酸在最大浓度下对谷氨酸诱导的HT22细胞死亡具有显着的神经保护作用。但是,对于M-3,M-6,M-7和M-10,几乎没有或几乎没有神经保护活性。我们目前的研究对于进一步了解它们在人类中的代谢命运和性状很重要。

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