基于《中华医典》文献挖掘中医治疗积聚的用药规律研究

目的:探讨《中华医典》中治疗积聚方剂的用药特点及其规律。方法:检索《中华医典》治疗积聚的方剂,按照纳入和排除标准筛选治疗积聚的方剂,建立Excel数据库,进行用药频次、性味、归经分析。并使用R语言arules包及arulesViz包对筛选处方中的药物进行关联规则分析及可视化,使用IBM SPSS Modeler 18.0对药物进行复杂网络分析,采用SPSS Statistics 26.0对聚类方剂进行分析。结果:筛选后共纳入方剂426首,包含中药303种,总用药频次4075次;四气9种,总频次3214次;五味8种,总频次5490次;十二经总频次11936次。治疗积聚应用频次较高的药物前3位为木香、肉桂、当归;关联性药对以三棱、木香出现频次最高。复杂网络分析,木香-肉桂、木香-三棱之间的关联性较强。聚类图谱显示,皮尔逊相关性为20时,高频药物可聚为5类。结论:历代医家在积聚治疗时,所用药物药性以温性为主,药味以辛味和苦味为主,归经侧重于脾胃经,功效以理气药、温里药、补益药为主。通过对《中华医典》中治疗积聚的用药规律研究,为临床实践中药治疗积聚相关疾病提供参考。

基于数据挖掘的《中华医典》中胁痛的组方用药规律研究

目的探析《中华医典》所载的治疗胁痛处方的用药规律。方法收集《中华医典》中治疗胁痛的处方,利用Excel(Microsoft Office 2019)录入处方数据及药物信息,对药物功效、四气五味、归经等进行频次统计。用SPSS Modeler 18.0及Cytoscape 3.9.1统计药物共现频次并进行可视化网络展示。用R语言arules包及arules Viz包对筛选处方中的药物进行关联规则分析及可视化,使用SPSS Statistics 19.0对高频药物进行聚类分析。结果共筛选出359首有效处方,使用中药240味,总用药频次3032次,核心药物有当归、甘草、白芍、柴胡、青皮、陈皮等,主要以补虚、理气、活血化瘀药三类药物为主。药物四气以温性为主,药物五味偏辛、苦、甘味,归经主要以脾、肝、肺、胃、心经为主。关联规则分析得到药物关联规则15组,以半夏,生姜与甘草的置信度最高,15组药物关联规则组合功效主要以补气、养血、行气、化瘀、除湿热为主。高频药物可以聚为5类,以疏肝解郁、清热燥湿、行气止痛、活血化瘀为主。结论《中华医典》记载治疗胁痛处方呈现以疏肝行气、活血化瘀、柔肝止痛、化痰燥湿、扶正补虚为主的组方规律,与胁痛的核心病机相符,为临床中医治疗胁痛提供参考。

基础专业课培养研究生科研创新能力探讨

创新能力培养是研究生科研能力培养的关键环节。文章旨在从研究生专业课教学课程改革入手,融入科研创新性培养内容,如进行科研课题综述、设计和解析高水平研究论文的创新点,使课堂呈现科研的创新氛围,以培养学生的创新意识。

一贯煎联合骨髓间充质干细胞调控RhoA/ROCK1通路抑制大鼠肝纤维化的实验研究

目的:探究一贯煎联合骨髓间充质干细胞在治疗肝纤维化过程中对RhoA/ROCK1通路的作用。方法:将72只SD大鼠随机分为正常对照组、模型对照组、秋水仙碱组、一贯煎高剂量组、一贯煎中剂量组、一贯煎低剂量组、干细胞组、一贯煎+干细胞组;四氯化碳腹腔注射6周制备肝纤维化动物模型,干预4周后取材。记录大鼠阴虚表征情况;检测血清谷丙转氨酶(GPT)、谷草转氨酶(GOT)含量;HE、Masson染色观察病理改变;实时PCR、蛋白质印迹法检测肝组织中RhoA、Rho相关激酶1(ROCK1)、α-SMA和COL-1 mRNA及蛋白表达;IHC检测α-SMA、COL-1阳性面积。结果:与正常对照组比较,模型对照组大鼠具有明显阴虚表征,肝脏出现明显炎症浸润和纤维增生,肝组织RhoA、ROCK1、α-SMA、胶原蛋白-1(COL-1)mRNA与蛋白表达显著升高(P<0.05),α-SMA、COL-1阳性面积显著增加(P<0.05);与模型对照组比较,一贯煎高剂量组、一贯煎中剂量组、一贯煎低剂量组、骨髓干细胞、一贯煎+干细胞组大鼠的阴虚表征、肝脏炎症和纤维化程度减轻,RhoA、ROCK1、α-SMA和COL-1 mRNA与蛋白表达显著降低(P<0.05),α-SMA、COL-1阳性面积显著减少(P<0.05),其中一贯煎+干细胞组较一贯煎中剂量组、干细胞组效果更优(P<0.05)。结论:一贯煎与骨髓干细胞可通过调控RhoA/ROCK1通路抑制肝星状细胞活化从而发挥抗纤维化的作用,二者协同作用效果优于各自单独作用效果。

高糖对H9C2心肌细胞系和乳大鼠心室肌细胞钙库操纵性钙内流及相关蛋白的影响

目的探究高糖环境对大鼠胚胎心肌细胞系(H9C2)和乳大鼠心室肌细胞(neonatal rat ventricular myocytes,NRVMs)钙库操纵性钙内流(store operated calcium entry,SOCE)功能的影响,对基质相互作用分子1(stromal interaction molecule 1,STIM1)蛋白表达及其激活结构的作用,完善SOCE在糖尿病心肌病(diabetic cardiomyopathy,DCM)中的潜在致病机制。方法将H9C2和NRVMs细胞分为2组,对照组(5.5 mmol/L葡萄糖)和高糖组(25 mmol/L葡萄糖),分别培养48 h后用激光共聚焦显微镜实时观察各组心肌细胞在毒胡萝卜素(thapsigargin,TG)刺激后Ca2+荧光强度值的变化;采用Western blotting技术检测各组细胞STIM1和钙释放激活钙通道调节分子1(calcium release-activated calcium channel modulator 1,Orai1)蛋白表达的变化;借助化学交联技术和免疫荧光法检测NRVMs的STIM1蛋白的聚集变化;免疫共沉淀技术观察NRVMs心肌细胞内源性STIM1和Orai1蛋白的直接相互作用。结果与对照组相比,高糖组H9C2和NRVMs心肌细胞钙内流(Ca2+ influx)显著增加(P<0.05);高糖组H9C2和NRVMs心肌细胞STIM1以及Orai1蛋白表达上调(P<0.01);钙库排空后,高糖组NRVMs心肌细胞STIM1蛋白聚集体显著增多(P<0.01)。结论体外高糖能诱导大鼠胚胎心肌细胞系H9C2及乳大鼠原代培养心室肌细胞NRVMs的STIM1和Orai1蛋白表达上调,促进STIM1蛋白激活形成聚集体和SOCE激活,Ca2+内流增多。该作用提示高糖增加的心肌细胞SOCE可能与糖尿病心肌肥大有关。

Protective effect of Yiguanjian decoction against DNA damage on concanavalin A-induced liver injury mice model

OBJECTIVE:To investigate the inhibitory effect of Yiguanjian decoction(YD) on DNA damage in Concanavalin A(Con A)-induced liver injury mice model and to explain the possible mechanism.METHODS:Totally 120 male BALB/c mice were randomly divided into 6 groups,20 mice each:normal group,model group,Bifendate group,YD low dose group,YD middle dose group and YD high dose group.Except normal group,liver injury model induced by Con A was established.While modeling,each mouse in YD group was given YD(0.4 m L/20 g per day) by intragastric administration(0.13 g YD for YD low dose group;0.26 g for YD middle dose group;0.52 g for YD high dose group).Bifendate group was given Bifendate(0.2 gnd model·kg-1 grou·d-1) by gavage.Normal group ap were fed with same volume of physiological saline daily.After 8 weeks,the serum alanine transaminase(ALT)and aspartate transaminase(AST) were tested.The hematoxylin-eosin staining was used to evaluate the grade of liver inflammation and liver fibrosis stage.Hepatocellular DNA damage was detected by single cell gel electrophoresis technology.The protein expression of tumor necrosis factor-α(TNF-α),Bax and Mut T Homolog 1(MTH1) was detected by western blotting and enzyme linked immunosorbent assay.Bax m RNA and MTH1 m RNA were detected by Real-time Polymerase Chain Reaction(PCR).RESULTS:YD can improve the degree of liver inflammation and fibrosis in the liver of chronic hepatitis mice,the dose effect relationship is remarkable(P < 0.05).YD can reduce liver cell DNA damage.The difference between YD middle dose group and model group was statistically significant(P < 0.05).YD middle dose group had decreased the protein expression of TNF-α in the mice liver of immunological liver injury(P < 0.05).YD can increase the protein expression of Bax(P < 0.05).Compared with normal group,the protein expression of MTH1 was decreased(P < 0.05),but there was no statistical significance between YD group and model group(P >0.05).YD can increase the m RNA expression of Bax and MTH1(both P < 0.05).CONCLUSION:YD can effectively inhibit the DNA damage in immunological liver injury mice,the mechanism may be that it can decrease the TNF-αand increase the Bax and MTH1 expression.