降糖提取物诱导糖尿病小鼠肝糖原积累的化学特性。

Garcia Gonzalez Jessica, Garcia Lorenzana Mario, Zamilpa Alejandro, Almanza Perez Julio Cesar, Jasso Villagomez E Ivan, Roman Ramos Ruben, Alarcon-Aguilar Francisco Javier
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引用次数: 18

摘要

背景:葫芦巴果实水提物具有降血糖作用,这可能与水提物中的某些成分有关。然而,这种水果的主要次生代谢物尚未确定,而且对其胰腺外的作用,特别是对肝脏碳水化合物代谢的作用知之甚少。因此,本研究除了对西葫芦水提物的主要成分进行分离和结构解析外,还旨在确定西葫芦水提物对糖尿病小鼠的降糖作用是否与肝糖原的积累有关。材料与方法:对枳实水提物进行分离纯化,并对其主要次生代谢产物进行化学表征(NMR和GC-MS)。四氧嘧啶诱导的糖尿病小鼠每天灌胃水提物(30 d)。采用光谱法和PAS染色法测定肝糖原含量;用光谱法测定ALT和AST;Western blot检测糖原合成酶、糖原磷酸化酶和GLUT2;RT-PCR检测GLUT2和胰高血糖素受体mRNA的表达;ELISA法测定血清胰岛素含量。H&E染色进行肝脏组织学分析。结果:对香豆酸、对羟基苯甲酸、水杨苷、柱头-7,2,2-二烯-3-醇和柱头-7-烯-3-醇5种化合物的化学指纹图谱显示为主要化合物。组织学分析显示肝糖原积聚。糖原合成酶升高,糖原磷酸化酶降低。有趣的是,组织学结构证明了提取物对肝脏的保护作用。结论:从水提物中鉴定出5个化合物。该提取物的降糖作用可能部分与肝糖原积累有关。该提取物降糖作用的生物活性化合物将在后续研究中进一步阐明。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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CHEMICAL CHARACTERIZATION OF A HYPOGLYCEMIC EXTRACT FROM CUCURBITA FICIFOLIA BOUCHE THAT INDUCES LIVER GLYCOGEN ACCUMULATION IN DIABETIC MICE.

Background: The aqueous extract of Cucurbita ficifolia (C. ficifolia) fruit has demonstrated hypoglycemic effect, which may be attributed to some components in the extract. However, the major secondary metabolites in this fruit have not yet been identified and little is known about its extra-pancreatic action, in particular, on liver carbohydrate metabolism. Therefore, in addition to the isolation and structural elucidation of the principal components in the aqueous extract of C. ficifolia, the aim of this study was to determine whether or not the hypoglycemic effect of the aqueous extract of Cucurbita ficifolia (C. ficifolia) fruit is due to accumulation of liver glycogen in diabetic mice.

Materials and methods: The aqueous extract from fruit of C. ficifolia was fractionated and its main secondary metabolites were purified and chemically characterized (NMR and GC-MS). Alloxan-induced diabetic mice received daily by gavage the aqueous extract (30 days). The liver glycogen content was quantified by spectroscopic method and by PAS stain; ALT and AST by spectrometric method; glycogen synthase, glycogen phosphorylase and GLUT2 by Western blot; the mRNA expression of GLUT2 and glucagon-receptor by RT-PCR; while serum insulin was quantified by ELISA method. A liver histological analysis was also performed by H&E stain.

Results: Chemical fingerprint showed five majoritarian compounds in the aqueous extract of C. ficifolia: p-coumaric acid, p-hydroxybenzoic acid, salicin, stigmast-7,2,2-dien-3-ol and stigmast-7-en-3-ol. The histological analysis showed accumulation of liver glycogen. Also, increased glycogen synthase and decreased glycogen phosphorylase were observed. Interestingly, the histological architecture evidenced a liver-protective effect due the extract.

Conclusion: Five compounds were identified in C. ficifolia aqueous extract. The hypoglycemic effect of this extract may be partially explained by liver glycogen accumulation. The bioactive compound responsible for the hypoglycemic effect of this extract will be elucidated in subsequent studies.

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