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番荔枝枝的抗溃疡成分。

Anti-ulcer constituents of Annona squamosa twigs.

机构信息

Division of Medicinal and Process Chemistry, Central Drug Research Institute, CSIR, Lucknow 226001, India.

出版信息

Fitoterapia. 2011 Jun;82(4):666-75. doi: 10.1016/j.fitote.2011.02.005. Epub 2011 Feb 20.

DOI:10.1016/j.fitote.2011.02.005
PMID:21342663
Abstract

Phytochemical investigation of Annona squamosa twigs, resulted in isolation and identification of twelve known (1-12) compounds among them one 1-(4-β-D-glucopyranosyloxyphenyl)-2-(β-D-glucopyranosyloxy)-ethane (11) is synthetically known but first time isolated from natural sources. Their structures were elucidated using 1D and 2D NMR spectroscopic analysis. The isolated compounds (2-8, 11) were evaluated for H(+) K(+)-ATPase activity. Three of these compounds (+)-O-methylarmepavine (2), N-methylcorydaldine (3), isocorydine (6) showed promising anti-secretory activity. Activity of these compounds, comparable to the standard drug omeprazole is novel to our finding. Moreover, there is no information accessible regarding the pharmacological effect of A. squamosa on the gastrointestinal system. This study is the first of its kind to show the significant anti-ulcer effect of A. squamosa. The present study aimed to evaluate the gastroprotective effect of A. squamosa (AS) and to identify its active constituents. Anti-ulcer activity was evaluated against cold restraint (CRU), pyloric ligation (PL), aspirin (ASP), alcohol (AL) induced gastric ulcer and histamine (HA) induced duodenal ulcer model and further confirmed through in vitro assay of H(+) K(+)-ATPase activity and plasma gastrin level. AS and its chloroform and hexane fraction attenuated ulcer formation in CRU, PL, HA model and displayed anti-secretory activity in vivo through reduced free, total acidity and pepsin in PL, confirmed by in vitro inhibition of H(+) K(+)-ATPase activity with corresponding decrease in plasma gastrin level. Cytoprotection of AS was apparent with protection in AL, ASP models and enhanced mucin level in PL.

摘要

番荔枝小枝的植物化学研究,导致分离和鉴定 12 种已知化合物(1-12),其中一种 1-(4-β-D-吡喃葡萄糖基氧苯基)-2-(β-D-吡喃葡萄糖基氧基)乙烷(11)是合成已知的,但首次从天然来源中分离出来。它们的结构是通过 1D 和 2D NMR 光谱分析阐明的。分离得到的化合物(2-8、11)被评估了 H(+) K(+)-ATP 酶活性。其中三种化合物(+)-O-甲基阿朴啡(2)、N-甲基考利定(3)、异考定(6)表现出有希望的抗分泌活性。这些化合物的活性与标准药物奥美拉唑相当,这是我们发现的新现象。此外,关于番荔枝对胃肠道的药理作用,目前还没有相关信息。这项研究是首次表明番荔枝具有显著的抗溃疡作用。本研究旨在评估番荔枝(AS)的胃保护作用,并鉴定其活性成分。抗溃疡活性通过冷束缚(CRU)、幽门结扎(PL)、阿司匹林(ASP)、酒精(AL)诱导的胃溃疡和组胺(HA)诱导的十二指肠溃疡模型进行评估,并通过体外 H(+) K(+)-ATP 酶活性和血浆胃泌素水平进一步确认。AS 及其氯仿和正己烷部分减轻了 CRU、PL、HA 模型中的溃疡形成,并通过降低 PL 中的游离、总酸度和胃蛋白酶显示出体内抗分泌活性,这通过体外抑制 H(+) K(+)-ATP 酶活性和相应降低血浆胃泌素水平得到证实。AS 的细胞保护作用明显,在 AL、ASP 模型中具有保护作用,并在 PL 中增强了粘蛋白水平。

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