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香青兰(唇形科香青属)的化学成分和心脏活性

Chemical composition and cardiotropic activity of Ziziphora clinopodioides subsp. bungeana (Juz.) Rech.f.

机构信息

Saint Petersburg State Chemical Pharmaceutical University, Saint Petersburg, Department of Pharmacognosy, Russia.

Saint Petersburg State Chemical Pharmaceutical University, Saint Petersburg, Department of Pharmacology and Clinical Pharmacology, Russia.

出版信息

J Ethnopharmacol. 2023 Oct 28;315:116660. doi: 10.1016/j.jep.2023.116660. Epub 2023 May 28.

Abstract

ETHNOPHARMACOLOGICAL RELEVANCE

Ziziphora clinopodioides subsp. bungeana (Juz.) Rech.f. is a subshrub that is widely distributed in China, Kazakhstan, Kyrgyzstan, Mongolia, Russia, Tajikistan, Turkmenistan, and Uzbekistan. The species is used in traditional medicine for the relief of symptoms connected to cardiovascular diseases like coronary heart disease or hypertension.

AIM OF THE STUDY

was to validate traditional use of Z. clinopodioides subsp. bungeana for the treatment of coronary hearth diseases using in vivo models and to find active compounds responsible for the activity.

MATERIALS AND METHODS

Multiple extracts were obtained from the aerial parts of Z. clinopodioides subsp. bungeana using maceration, liquid-liquid extraction, CO2 extraction and ultrasound-assisted extraction. Preliminary screening studies for the evaluation of the efficacy of Z. clinopodioides subsp. bungeana extracts on the model of hemic hypoxia were performed. The most effective samples were selected and included in the main study. Stage 2 of the study evaluated the cardiotropic activity of the selected extracts on a model of chronic heart failure. Preparations were administered to animals intragastrically once a day for 28 days. For the isolation of individual compounds plant material was extracted with 96% ethanol. The obtained crude extract was sequentially extracted with n-hexane and dichloromethane and separated by chromatography on a Diaion HP-20 column. The obtained fractions were further subjected to Sephadex LH-20 column chromatography and eluted isocratically with 96% ethanol (EtOH) to yield subfractions, which were further separated by preparative HPLC to obtain 13 individual compounds.

RESULTS

Extracts obtained from Ziziphora clinopodioides subsp. bungeana (Juz.) Rech.f. herb were subjected to pharmacological screening for the evaluation of their efficacy on hemic hypoxia. Based on the obtained results, out of the sixteen tested extracts two (AR and US 60%) were selected for further evaluation of their cardiotropic activity. Modeling of chronic heart failure was carried out in accordance with the following stages: 1) anesthesia with chloral hydrate at a dose of 450 mg/kg, intraperitoneally, 2) artificial ventilation of the lungs, 3) thoracotomy, 4) modeling of permanent ischemic or ischemic-reperfusion damage. Both extracts effected the indicators of contraction and output, comparable to the reference drug - Monopril. Based on the extraction methods used to obtain RAF and US60 and data from the literature, it can be assumed that they contain compounds with medium polarity, including polyphenols and terpenoids. At the next stage three previously undescribed monoterpenoid derivatives - Ziziphoric acid (1), Ziziphoroside D (2) and 6'-malonylziziphoroside A (3), along with two previously described megastigmane glucosides - blumenol C glucoside (4), blumenol C 9-O-(6'-O-malonyl-beta-D-glucopyranoside (5) and two previously described monoterpenoids 7a-hydroxymintlactone (6), 7-hydroxypiperitone (7) together with six polyphenols - pinocembrine-7-O-rutinoside (8), chrysine-7-O-rutinoside (9), acacetin-7-O-rutinoside (10), luteolin-7-O-rutinoside (11), rutin (12) and rosmarinic acid (13) were isolated from Z. clinopodioides subsp. bungeana extracts.

CONCLUSION

Our results support the traditional use of Z. clinopodioides subsp. bungeana for the treatment of coronary diseases. As a result of Z. clinopodioides subsp. bungeana extracts screening in vivo, two extracts were selected as potential cardiotropic agents. Phytochemical analysis of the plant material led to the isolation of five terpenoid derivatives, two megastigmane glycosides, five flavonoids and one cinnamic acid derivative, which could be responsible for the reported biological activity. Future experiments are required to understand the mechanisms of action for the isolated compounds.

摘要

民族药理学相关性

密花香薷(Ziziphora clinopodioides subsp. bungeana (Juz.) Rech.f.)是一种广泛分布于中国、哈萨克斯坦、吉尔吉斯斯坦、蒙古、俄罗斯、塔吉克斯坦、土库曼斯坦和乌兹别克斯坦的亚灌木。该物种在传统医学中用于缓解与心血管疾病相关的症状,如冠心病或高血压。

研究目的

验证密花香薷(Z. clinopodioides subsp. bungeana)用于治疗冠心病的传统用途,使用体内模型寻找负责该活性的活性化合物。

材料和方法

使用浸渍法、液液萃取法、CO2 萃取法和超声辅助提取法从密花香薷(Z. clinopodioides subsp. bungeana)的地上部分获得多种提取物。进行初步筛选研究,以评估密花香薷(Z. clinopodioides subsp. bungeana)提取物对贫血模型的疗效。选择最有效的样品并将其包括在主要研究中。研究的第二阶段评估了所选提取物对慢性心力衰竭模型的心脏活性。制剂通过灌胃每天一次给药 28 天。为了分离个别化合物,用 96%乙醇提取植物材料。获得的粗提取物依次用正己烷和二氯甲烷萃取,并通过 Diaion HP-20 柱色谱分离。获得的馏分进一步通过 Sephadex LH-20 柱色谱洗脱,并以等度洗脱 96%乙醇(EtOH),得到亚馏分,然后通过制备 HPLC 进一步分离,得到 13 种单体化合物。

结果

从密花香薷(Ziziphora clinopodioides subsp. bungeana (Juz.) Rech.f.)植物中获得的提取物用于评估其对贫血的疗效的药理筛选。根据获得的结果,从十六种测试提取物中选择了两种(AR 和 US 60%)进行进一步评估其心脏活性。慢性心力衰竭的建模按照以下阶段进行:1)氯醛合剂量为 450mg/kg,腹膜内麻醉,2)肺人工通气,3)开胸,4)永久缺血或缺血再灌注损伤建模。两种提取物都影响收缩和输出的指标,与参考药物蒙诺普利相当。基于获得 RAF 和 US60 的提取方法和文献数据,可以假设它们含有中等极性的化合物,包括多酚和萜类化合物。在下一阶段,分离了三种以前未描述的单萜衍生物——密花香薷酸(1)、密花香薷甙 D(2)和 6'- 丙二酰基齐地索甙 A(3),以及两种以前描述的大根香叶素葡萄糖苷——blumenol C 葡萄糖苷(4)、blumenol C 9-O-(6'-O-丙二酰基-β-D-吡喃葡萄糖苷(5)和两种以前描述的单萜类化合物 7a-羟基薄荷内酯(6)、7-羟基胡椒酮(7),以及六种多酚类化合物——pinocembrine-7-O-芸香糖苷(8)、chrysine-7-O-芸香糖苷(9)、acacetin-7-O-芸香糖苷(10)、木犀草素-7-O-芸香糖苷(11)、芦丁(12)和迷迭香酸(13)。

结论

我们的结果支持密花香薷(Z. clinopodioides subsp. bungeana)用于治疗冠心病的传统用途。通过密花香薷(Z. clinopodioides subsp. bungeana)提取物的体内筛选,选择了两种提取物作为潜在的心脏活性药物。对植物材料的植物化学分析导致分离出五种萜类衍生物、两种大根香叶素糖苷、五种类黄酮和一种肉桂酸衍生物,这些化合物可能是报道的生物活性的原因。需要进一步的实验来了解分离化合物的作用机制。

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