Mechanism of Polygoni Cuspidati Rhizoma in treating atherosclerosis based on network pharmacology and molecular docking

Background:The incidence and prevalence of atherosclerosis(AS)is increasing every year and has becoming a major health issue of global concern.Polygoni Cuspidati Rhizoma(PCR)is a Chinese herb that is widely used clinically for the treating of AS.However,its pertinent targets and probable mechanisms,still need to be completely explored.Methods:Active compounds and targets for PCR and AS targets were screened using public databases.A“drug-component-disease target”network map was created and analyzed after using the Venn online tool to identify common targets and Cytoscape software to screen drug-disease core targets.Critical targets pathway enrichment analyses are conducted using the Metascape database.Using AutoDock Vina and Pymol software,docking validation and visualization of active components and core targets were carried out.Results:PCR was obtained for ten compounds with 105 AS-related targets.Rhein,quercetin,beta-sitosterol,and luteolin may be drug candidates,and the genes for AKT1,TNF,IL-6,EGFR,TP53,IL-1,RELA,and VEGFA are potential therapeutic targets,according to network analysis.PCR might modulate the AGE/RAGE,PI3K/Akt,IL-17 and NF-ᴋB signaling pathways against the development of AS.Molecular docking indicated that quercetin has high affinity for AKT1 and TNF gene targets.Conclusion:This study provides rare information and scientific basis for further exploration of PC in the treatment of AS.

A high expression EGFR/cell membrane chromatography and online high performance liquid chromatography/mass spectrometry method for screening EGFR antagonists from Rhizoma Polygoni Cuspidati

The epidermal growth factor receptors(EGFRs)in some tumor cells are significant targets for drug discovery.In this work,we have developed an EGFR cell membrane chromatography and online high performance liquid chromatography/mass spectrometry system for screening active component from Rhizoma Polygoni Cuspidati.As a result,resveratrol from Rhizoma Polygoni Cuspidati was found to be the active component acting on EGFR like gefitinib.There was a good relationship between their inhibiting effects on EGFR secretion and HEK293 EGFR cell growth in vitro.The EGFR/CMC-online-HPLC/MS system demonstrated fast and effective characteristics for screening leading compounds from traditional Chinese medicine.

Effect of Polygoni Cuspidati Rhizoma et Radix and Its Ingredient Resveratrol on Experimental Autoimmune Myasthenia Gravis by Suppressing Immune Response

Objective To investigate the effects of Polygoni Cuspidati Rhizoma et Radix （PCRR） and its ingredient resveratrol （Res） on experimental autoimmune myasthenia gravis （EAMG）. Methods EAMG was induced in Lewis rats by the immunization of a synthetic peptide corresponding to region 97-116 of the rat acetylcholine receptor （AChR） α subunit （R97-116）. EAMG rats were randomly divided into PCRR group, Res group, and control （C） group, and were ig administered respectively with PCRR （2 g/kg）, Res （20 mg/kg）, and DMSO （0.4 mL/kg） every day from day 5 after immunization to day 42. Clinical evaluation, lymphocyte proliferation, cytokines, and anti-97-116 antibodies were performed for examination of their therapeutic effects. Results Treatments with PCRR and Res significantly ameliorated clinical symptoms, down-regulated TNF-α and up-regulated IL-10 in serum and culture supernatants of lymphocytes stimulated with R97-116, and decreased levels of anti-R97-116 IgG1 and IgG2a in serum compared with C group. Unexpectedly, PCRR but not Res inhibited lymphocyte proliferation compared with C group. Conclusion PCRR and Res ameliorating EAMG is associated with suppressing immune response, and indicates a therapeutic potential for EAMG and even human myasthenia gravis （MG）. Res may be the main effective ingredient from PCRR ameliorating EAMG, but further experiments are necessary.

Effect of Rhizoma Polygoni Cuspidati and Ramulus Cinnamomi Compatibility on Uric Acid Metabolism and Urinary Neutrophil Gelatinase-Associated Lipocalin and Kidney Injury Molecule-1 in Rats with Hyperuricemia

Objective：To explore the effects of Rhizoma Polygoni Cuspidati and Ramulus Cinnamomicompatibility（PR） on uric acid metabolism and the expression of urinary neutrophil gelatinase-associated lipocalin（NGAL） and kidney injury molecule-1（KIM-1） in rats with hyperuricemia. Methods：Seventy male Sprague Dawley（SD） rats were randomly divided into 7 groups with 10 rats per group, including the normal group, model group, allopurinol group, benzbromarone group and PR groups at 3 doses（3.5, 7, 14 g/kg）. Except the normal group, rats of the other groups were intragastrically administered 100 mg/kg hypoxanthine and 250 mg/kg ethambutol, and subcutaneously injected with 200 mg/kg potassium oxonate. All rats were continuously modeled for 17 days, and gavaged with corresponding drugs. The rats of the normal and model groups were gavaged with saline, once a day, for 2 weeks. The levels of serum uric acid（SUA）, blood urea nitrogen（BUN） and creatinine（Cr） were determined. In addition, the contents of NGAL and KIM-1 in urine and the m RNA and protein expressions of xanthine oxidase（XOD） in liver of hyperuricemia rats were measured by reverse transcription polymerase chain reaction（RT-PCR） and Western blot, respectively. Moreover, the pathological changes of kidney were analyzed by hematoxylin and eosin（HE） stain method. Results：Compared with the normal group, the levels of SUA, BUN, NGAL and KIM-1 and the expressions of hepatic XOD m RNA and protein in the hyperuricemia rats were increased significantly（P〈0.01）. PR significantly decreased the levels of SUA, BUN, NGAL and KIM-1 and down-regulated the m RNA and protein expressions of hepatic XOD（P〈0.05 or P〈0.01）. In addition, the pathological changes of kidney were significantly suppressed by oral administration of PR. Conclusions：PR ameliorated uric acid metabolism and protected renal function, the underlying mechanism was mediated by decreasing the levels of SUA, BUN, NGAL and KIM-1, inhibiting the expression of hepatic XOD and ameliorating the pathological change of kidney.

基于水负荷动物模型及生物信息学虎杖利湿作用的初步研究

目的:通过制备小鼠水负荷模型观察虎杖的利湿作用,并基于生物信息学初步探讨其发挥作用的物质基础及可能机制。方法:设置虎杖水提液不同剂量组(9.2、4.6、2.3 g·kg^(-1))构建小鼠水负荷模型;采用ICP-OES法测定小鼠尿液中的钠钾离子浓度;在TCMSP数据库预测虎杖活性成分靶点,Genecards数据库获取湿病相关靶标;取两者交集构建PPI网络并优化,利用Cytoscape3.8.0软件构建“药物-成分-靶点-疾病-通路”网络;在DAVID6.8数据库富集分析交集靶点;借助AutoDock Tools-1.5.7软件进行分子对接。结果:实验表明虎杖水提液中剂量组(4.6 g·kg^(-1))利尿效果显著(P<0.05),可促进钠、钾离子排泄。网络数据库及软件高通量分支和整体筛选中获取虎杖活性成分27个,药物和湿病交集靶点275个;核心靶点为STAT3、TP53、SRC;活性成分包括芹菜素、木犀草素、槲皮素等;相关通路主要涉及AGE-RAGE信号通路、催乳素信号通路、HIF-1信号通路。结论:通过网络可视图及网络组学分析技术初步预测了虎杖发挥利湿作用的关键成分、靶点及相关通路,可为其利湿功效的物质基础研究和临床应用提供理论依据。

白藜芦醇对小鼠艾滋病治疗作用的实验研究

【目的】观察中药虎杖提取物白藜芦醇的体内抗小鼠艾滋病病毒作用。【方法】BALB／C小鼠50只,随机分成正常组, 模型组,白藜芦醇高、低剂量组(剂量分别为20、4 mg·kg-1·d-1),齐多呋定(AZT)组(剂量为100mg·kg-1·d-1);除正常组外,其他组小鼠均腹腔接种Friend型鼠白血病病毒(FLV),复制小鼠艾滋病模型;病毒攻击后1 d,各组均按设计剂量给药,连续21 d;剖杀小鼠,观察白藜芦醇对模型小鼠的脾指数(质量比)及脾指数抑制率、胸腺指数(质量比)、外周血白细胞和红细胞计数以及CD3+、CD4+、CD8+T淋巴细胞亚群水平的影响。【结果】白藜芦醇高剂量组能抑制模型小鼠的脾肿大(P<0．05)和胸腺萎缩(P<0．01),升高外周血CD3+、CD4+、CD8+T淋巴细胞亚群水平(P<0．05或P<0．01), 与模型组比较差异均具有显著性意义。但对外周血的白细胞和红细胞数量未见显著性影响。【结论】白藜芦醇具有一定的体内抗小鼠艾滋病病毒作用。

虎杖商品药材中白藜芦醇苷的含量测定

目的 :改善虎杖药材中白藜芦醇苷含量测定的方法 ,并对不同来源商品药材进行测定。方法 :高效液相色谱法 ,C18柱为固定相 ,乙腈 水 (2 0∶80 )作为流动相 ,检测波长为 30 3nm ,流速 1mL·min-1。结果 :白藜芦醇苷在 0 .0 0 6 6～ 0 .0 792 μg·μL-1浓度范围内呈现良好的线性关系 ,相关系数r =0 .9999(n =5 ) ;平均回收率为98.5 % ,RSD为 2 .5 % (n =9)。结论 :该方法简单、准确 ,重现性好。不同来源商品药材测定结果表明 ,白藜芦醇苷含量最高达到 3.6 3% ,最低为 1.2 0 % ,平均含量为 2 .2 3% ,差异并不十分悬殊。

虎杖对肺纤维化大鼠肺组织中TGF-β_1表达的影响

目的:观察博莱霉素致肺纤维化大鼠中转化生长因子(TGF-β1)的表达及虎杖对其影响。方法:SD大鼠120只,随机分成正常对照组、模型组、虎杖预防组各30只,7d治疗组20只和28d治疗组10只。除正常对照组给予生理盐水外,其余各组均予气管内注射博来霉素诱导肺纤维化。虎杖预防组、7d治疗组和28d治疗组胃饲受试药物4g.kg-1.d-1,其余两组则予生理盐水灌胃。用RT-PCR和免疫组化观察各组大鼠肺组织TGF-β1mRNA和TGF-β1蛋白的表达。结果:与模型组比较,虎杖预防组和7d治疗组羟脯氨酸含量下降明显(P<0.05或P<0.01),TGF-β1mRNA和TGF-β1蛋白表达较模型组减弱(P<0.05或P<0.01)。结论:虎杖抑制肺组织中TGF-β1的表达,可能是虎杖抑制肺纤维化的作用机制之一。

微波辅助提取石蒜和虎杖中有效成分的热力学机理研究

采用微波辅助提取(MAE)技术研究了石蒜和虎杖两种不同植物中石蒜碱、力可拉敏和加兰他敏以及白藜芦醇和大黄素提取过程的热力学机理.以溶剂回流提取方法(SRE)作为对比,采用一种简单的测定提取分配系数的方法,计算了这些组分在两种提取过程中的热力学函数ΔH0,ΔS0和ΔG0,对其化学结构与极性以及在MAE过程中的热力学行为进行了讨论,并用扫描电镜法观察了MAE和SRE提取后样品的细胞结构.结果表明,石蒜和虎杖的提取是一个吸热熵增的过程,微波的作用导致石蒜和虎杖细胞结构发生显著变化,使MAE热力学函数变化较大,其提取过程的热力学行为特征与SRE明显不同,但提取效率提高.

虎杖药材指纹图谱研究

目的应用RP-HPLC对不同产地虎杖药材进行指纹图谱研究。方法K rom as il C18色谱柱(150 mm×4.6mm,5μm),乙腈-水二元梯度洗脱,体积流量:1 mL/m in,检测波长303 nm。结果根据选择的色谱条件制订了不同产地虎杖药材的指纹图谱。结论色谱图对各产地虎杖药材中各成分得到了很好的分离,可作为虎杖药材的专属性指纹图谱。

18味中药提取物体外抗鸭瘟病毒活性的研究

我国传统中药在临床中广泛用于抗病毒疾病的治疗,该研究以18味传统中药为研究对象,希望找到对鸭瘟病毒具有良好抑制作用的中药原料。首先,通过细胞病变观察法(cytopathic effect,CPE)初步筛选了18味中药水提取物和醇提物进行体外抗鸭瘟病毒活性研究,发现当虎杖醇提物质量浓度为0.062 5mg/mL和0.031 3mg/mL,茜草醇提物质量浓度为0.007 8mg/mL时,可抑制鸭瘟病毒引起的鸭胚成纤维细胞病变。进而通过四甲基偶氮唑盐法[3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide,MTT]进一步研究了虎杖和茜草醇提物的体外抗鸭瘟病毒活性。结果显示:当虎杖质量浓度为0.062 5mg/mL、茜草质量浓度为0.007 8mg/mL时,对鸭瘟病毒的体外抑制率分别为76.50%、48.91%,虎杖醇提物的半数有效质量浓度(50%inhibitory concentration,IC50)为0.022 7mg/mL,茜草醇提物的IC50>0.007 8mg/mL。提示虎杖和茜草醇提物均有不同程度的体外抗鸭瘟病毒活性,其中虎杖效果优于茜草,具有进一步研究的价值。

虎杖升麻升高白细胞作用的实验研究

用昆明系小鼠，对虎杖升麻水煎液升高外周血白细胞的作用进行了实验研究。结果表明，虎杖升麻水煎液在正常生理条件下，并不引起实验动物白细胞的增加。对环磷酰胺所致白细胞减少的动物，在５５．０ｇ／ｋｇ的剂量下，使白细胞总数从６．２２×１０９／Ｌ上升到１２．８５×１０９／Ｌ。同时观察到白细胞总数的增加，主要是中性白细胞的升高。

虎杖提取液对非酒精性脂肪肝大鼠肿瘤坏死因子α基因表达的影响

应用RT qPCR方法检测分析非酒精性脂肪肝动物模型药物干预效果。经过4周的干预试验,干预组大鼠脂肪组织的TNF-αmRNA相对水平比对照组显著下降(t=2.452,P=0.022)。干预组的肝组织甘油三酯、总胆固醇和葡萄糖含量均低于对照组,其中总胆固醇含量的差异显著(t=2.555,P=0.019)。研究表明,虎杖水提液可以显著地降低NAFLD大鼠脂肪组织的TNF-αmRNA水平,也可以降低大鼠肝组织甘油三酯、总胆固醇和葡萄糖的含量,在调节肝脂、肝糖代谢和改善肝细胞脂肪变性具有一定效果。

复方虎杖提取物对高脂血症模型大鼠血脂水平和动脉硬化指数的影响

目的观察复方虎杖提取物对高脂饲料致高脂血症模型大鼠体质量、血脂水平和动脉硬化指数的影响。方法采用高脂饲料喂养SD大鼠建立高脂血症模型,灌胃给予复方虎杖提取物低、中、高剂量(4,8,12g·kg-1),连续8周。分别于给药第2,4,6,8周取血,测血清总胆固醇(TC)、甘油三酯(TG)及高密度脂蛋白胆固醇(HDL-c)、低密度脂蛋白胆固醇(LDL-c)含量及动脉粥样硬化指数(AI)。结果与模型组比较,复方虎杖提取物灌胃给予大鼠4周后即出现明显降血脂作用,除低剂量组AI外,其余各剂量组TC、TG、LDL-c及AI明显降低(P<0.01,P<0.05)。给药8周,低剂量组TC、LDL-c及AI明显降低(P<0.01);中剂量组血清TC、LDL-c及AI明显降低(P<0.01,P<0.05),HDL-c明显升高(P<0.05);高剂量组AI明显降低(P<0.01),HDL-c明显升高(P<0.05)。结论复方虎杖提取物4,8,12 g·kg-13个剂量组均可以改善高脂饲料致高脂血症模型大鼠的血清血脂水平,具有一定的降血脂作用,且高、中剂量组效果优于低剂量组。

虎杖—桂枝药对配伍对急性痛风性关节炎大鼠TLR4/MyD88信号转导通路的影响

【目的】观察虎杖—桂枝药对(虎桂药对)配伍对尿酸钠诱导的急性痛风性关节炎大鼠Toll样受体4/骨髓样分化因子88(TLR4/My D88)通路的影响,进一步探讨虎桂药对治疗急性痛风的作用机制。【方法】将SD雄性大鼠48只分为正常组、模型组、阴性质粒组、阳性质粒组、虎桂药对(剂量为7 g/kg)+si RNA组、虎桂药对组(剂量为7 g/kg),每组各8只。虎桂药对配伍组给予相应药物灌胃,其他各组给予生理盐水灌胃,每日1次,连续10 d。于灌胃第7天模型组和各实验组大鼠均采用踝关节腔内注射尿酸钠复制大鼠急性痛风性关节炎模型,正常组给予同体积的生理盐水;阳性质粒组、虎桂药对﹢si RNA组通过构建好的靶向TLR4基因si RNA(TLR4-si RNA)质粒抑制大鼠体内TLR4基因的表达。观察各组大鼠关节滑膜组织病理形态学变化,采用双抗体夹心法检测外周血炎症因子肿瘤坏死因子-α(TNF-α)和白细胞介素-1β(IL-1β)的含量,采用荧光定量PCR和Western blot法检测各组大鼠外周血单核细胞中TLR4、My D88、肿瘤坏死因子受体相关因子6(TRAF-6)m RNA和蛋白表达,免疫组织化学法检测滑膜核转录因子-κB p65(NF-κB p65)的表达。【结果】与正常组比较,模型组滑膜细胞明显增生,内膜下层炎细胞弥漫浸润,以淋巴、单核细胞为主,滑膜表面见大量纤维素粘附。与模型组比较,阳性质粒组,虎桂药对+si RNA组、虎桂药对组均能明显缓解炎性细胞对滑膜的浸润,改善滑膜细胞增生反应。与正常组比较,模型组血清TNF-α、IL-1β含量显著升高(P<0.01),外周血单核细胞TLR4、My D88、TRAF-6 m RNA和蛋白表达,滑膜NF-κB p65表达均显著升高(P<0.01);与模型组比较,阳性质粒组,虎桂药对+si RNA组、虎桂药对组血清中的TNF-α、IL-1β含量显著降低(P<0.01),外周血单核细胞TLR4、My D88、TRAF-6 m RNA和蛋白表达以及滑膜NF-κB p65表达均显著降低(P<0.05或P<0.01)。【结论】虎桂药对配伍具有调节细胞因子的作用,其机制可能与其抑制TLR4-My D88-NF-κB信号通路的异常激活有关。

虎杖药材高效毛细管电泳指纹图谱研究

目的:建立虎杖药材指纹图谱分析方法。方法:采用 Agilent^(3D)CE 高效毛细管电泳仪,未涂渍熔融石英毛细管(75μm×48.5cm,有效长度40.0cm),压力进样5.25Pa×3s,运行缓冲液为10mmol.L^(-1)硼酸钠溶液-甲醇(1:1),检测波长为220nm,运行电压30kV,温度25℃,内标为厚朴酚。结果:确定了虎杖药材甲醇提取部分12个共有峰,不同产地虎杖样品指纹图谱与对照指纹图谱相似度系数均在0.9以上,可用于虎杖药材的定性鉴别。结论:方法准确可靠,为提高虎杖药材质量控制标准提供参考。

微波辅助提取石蒜和虎杖中有效成分的动力学模型

基于微波辅助提取(MAE)中药材中化学成分的非稳态扩散过程,根据Fick第二定律建立了石蒜中石蒜碱、力可拉敏和加兰他敏以及虎杖中白藜芦醇和大黄素微波辅助提取过程的动力学模型.研究了提取时间、提取温度及药材粒度等因素对石蒜中石蒜碱、力可拉敏和加兰他敏以及虎杖中大黄素和白藜芦醇的提取率的影响,采用Matlab软件编程对动力学模型进行回归分析,拟合的动力学模型与实验结果吻合.根据模型计算了石蒜中石蒜碱、力可拉敏和加兰他敏以及虎杖中大黄素和白藜芦醇在MAE提取过程中的扩散系数D,与溶剂加热回流法(SRE)比较,引入增强因子γ,表征了微波对溶质分子扩散传质的影响及其对不同基质药材作用的差异.

几种中药的化学振荡指纹图谱

应用振荡技术 ,采用KBrO3 MnSO4 H2 SO4 丙酮振荡器 ,得到了解表药柴胡、葛根、连翘 ,祛风湿药木瓜、独活、五加皮和理血药鸡血藤、丹参、虎杖的振荡指纹图谱。结果表明 。

虎杖及配伍醇提液不同极性提取物的抑菌活性

对虎杖不同部位及其与蒲公英、北败酱、半枝莲配伍后抑菌活性进行了研究。用不同溶剂提取虎杖药材,再用不同极性的溶剂萃取虎杖及其配伍后的提取液,测定其对大肠杆菌、金黄色葡萄球菌、枯草杆菌、四联球菌和产气杆菌的抑菌活性。结果发现,虎杖醇提液抑菌活性大于水提液,其醇提取液的三氯甲烷部分抑菌活性最强,对以上5种细菌的最低抑菌浓度分布在0.0625-0.5 g.mL^-1。配伍后的三氯甲烷部分和正丁醇部分的抑菌活性较强。