桃红逐瘀汤治疗偏头痛40例疗效观察

目的:观察桃红逐瘀汤治疗偏头痛的疗效。方法:78例偏头痛患者随机分为治疗组40例和对照组38例。对照组给予盐酸氟桂利嗪胶囊2粒,睡前服1次。急性发作期加服麦角胺咖啡因片。治疗组在对照组治疗的基础上加用桃红逐瘀汤,每日1剂,水煎后分早晚服。两组均连续服用1个月。治疗前后监测偏头痛发作频率、持续时间、严重程度、伴随症状及血流变学指标。结果:治疗组总有效率显著高于对照组(P<0.05);血流变学五项指标的变化:治疗组治疗前后相比有显著性差异(P<0.05),对照组治疗前后相比无显著性差异(P>0.05);服用桃红逐瘀汤未发现明显的不良反应。结论:在西医治疗的基础上加用桃红逐瘀汤治疗偏头痛效果显著,安全性好。

桃红大将逐瘀汤对急性腰痛症疼痛缓解及便秘预防的疗效观察

[目的]观察桃红大将逐瘀汤对急性腰痛症疼痛缓解及便秘预防的疗效。[方法]将500例患者分为3组,桃红大将逐瘀汤组口服桃红大将逐瘀汤,甘露醇组口服甘露醇,芬必得组口服芬必得,同时配合中药外敷,静滴改善微循环药以及功能锻炼等,均治疗3天后观察疗效。[结果]在疼痛缓解方面桃红大将逐瘀汤明显优于其他两组,差异有统计学意义(P<0.01);在预防便秘方面桃红大将逐瘀汤组与甘露醇组疗效相近(P>0.05),两组均明显优于芬必得组(P<0.01)。[结论]桃红大将逐瘀汤治疗急性腰痛症疼痛及预防便秘方面临床运用安全、有效,并符合简、便、廉原则,便于临床推广。

桃红大将逐瘀汤加减方治疗胸腰椎骨折早期并发症73例

目的:观察桃红大将逐瘀汤加减方治疗胸腰椎骨折早期并发症的疗效。方法:73例无脊髓操作的胸腰椎骨折患者,给予桃红大将逐瘀汤加减方治疗。结果:治愈50例,显效12例,有效7例,无效4例,总有效率94.52%。结论:桃红大将逐瘀汤加减方治疗胸腰椎骨折早期并发症腹痛腹胀便秘效果甚佳,能尽早缓解病痛,缩短病程,有利于早日康复。

补肾祛痹汤配合手法治疗老年性膝骨性关节炎106例

目的:观察补肾壮骨,活血祛痹类中药内服外用配合手法治疗老年性膝骨性关节炎的疗效。方法:自拟补肾祛痹汤(人参、黄芪、熟地、枣皮、麻黄、防风、附子、细辛、薏仁、防己、地龙等)内服,外用桃红逐瘀汤(桃仁、红花、当归、地龙、乳香、没药、香附、牛膝、鸡血藤等)熏蒸外洗,配合手法松解粘连,松筋止痛治疗本病106例。结果:治愈率37.7%,总有效率92.6%。提示:本方法治疗本病有强筋骨,祛外邪,通经络,散痹痛的功效。

桃红大将逐瘀汤加减对颅脑损伤慢传输型便秘患者疗效观察

观察桃红大将逐瘀汤加减对颅脑损伤慢传输型便秘患者的临床效果。方法 采用随机数字表法将符合纳排标准的研究对象分为对照组(枸橼酸莫沙必利片)和试验组(桃红大将逐瘀汤加减)。接着使用便秘主症积分法对所用研究对象进行治疗前后量化评估,并运用SPSS 26.0软件进行统计分析。最后对两组分别进行治疗前后组内对照和组间对照分析。结果 治疗前,两组组间比较无明显差异(P>0.05);治疗后,两组积分较治疗前均有下降,组内比较有明显差异(P<0.05),但组间比较无明显差异(P>0.05);就治疗率而言,试验组优于对照组。结论 桃红大将逐瘀汤加减对颅脑损伤慢传输型便秘患者具有一定的临床疗效。

基于网络药理学探讨桃红大将逐瘀汤加减治疗便秘的作用机制

目的基于网络药理学探讨桃红大将逐瘀汤加减治疗便秘的作用机制。方法采用TCMSP数据库检索和筛选桃红大将逐瘀汤加减的中药活性化合物及其靶点;运用GeneGards和OMIM数据库筛选出与便秘相关的基因,将其与药物靶点交集获得靶基因并构建活性化合物-靶基因网络。利用String数据库构建靶基因的PPI网络,并筛选出关键基因;再对靶基因进行GO和KEGG富集分析。结果桃红大将逐瘀汤加减有82个活性化合物作用于227个基因,与疾病相关的基因有4663个,通过交集得到177靶基因;其中ALB、AKT1、IL6、JUN、CASP3、VEGFA、IL1B、EGFR、PTGS2、MYC等10个基因是关键基因,主要富集在169个GO条目以及IL-17信号通路、TNF信号通路等158个KEGG通路中。结论桃红大将逐瘀汤加减主要通过ALB、AKT1、IL6等基因及IL-17信号通路和TNF信号通路调节肠道蠕动功能,达到治疗便秘目的。

Comparison of mechanisms and efficacies of five formulas for improving blood circulation and removing blood stasis

Objective This study aimed to compare the mechanisms and efficacies of five formulas that improve blood circulation and remove blood stasis.Methods(1)A network pharmacology method was used to determine the targets of five formulas that promote circulation and remove blood stasis.Compounds of the five formulas,namely Danshen Yin(丹参饮,DSY),Huoluo Xiaoling Dan(活络效灵丹,HLXLD),Shixiao San(失笑散,SXS),Taohong Siwu Tang(桃红四物汤,THSWT),and Xuefu Zhuyu Tang(血府逐瘀汤,XFZYT),were retrieved from the Traditonal Chinese Medicine System Pharmacology Database(TCMSP),the Shanghai Institute of Organic Chemistry of CAS,and the TCM Integrated Database.Drug target network was constructed by searching the Swiss Target Prediction database and the STITCH database.The target network of stasis was extracted from the PharmGKB database,the Online Mendelian Inheritance in Man(OMIM)database,the Genetic Association Database(GAD),and the Therapeutic Target Database(TTD).Candidate targets were determined using protein-protein interaction(PPI)network extension and topology selection.Thereafter,Kyoto Encyclopedia of Genes and Genomes(KEGG)enrichment analysis was used to determine the differentiation of the mechanism of the five formulas.(2)Animal experiments were conducted to explore the efficacies of the five formulas in treating blood stasis.Seventy New Zealand rabbits were exposed to high-fat feeding+epinephrine injection to construct a blood stasis syndrome model.The rabbits were evenly divided into control,model,DSY,HLXLD,SXS,THSWT,and XFZYT groups.The latter five groups were orally administered the corresponding formulas[DSY:3.92 g/(kg·d),XFZYT:7.10 g/(kg·d),SXS:1.12 g/(kg·d),HLXLD:5.60 g/(kg·d),THSWT:4.48 g/(kg·d)].Serum lipid and blood rheology were analyzed,and pathology slices were observed.Results(1)A total of 269,358,288,370,and 376 candidate targets of DSY,HLXLD,SXS,THSWT,and XFZYT were obtained among which were 232 shared candidate targets.Fluid shear stress and atherosclerosis were the biological processes common to the five formulas.HLXLD,SXS,DSY,and THSWT regulated lipolysis in adipocytes,and XFZYT,HLXLD,SXS,and THSWT regulated the AGE-RAGE signaling pathway and complement and coagulation cascades.HLXLD,SXS,and XFZYT regulated the HIF-1 signaling pathway,DSY regulated the cGMP-PKG signaling pathway,HLXLD reduced platelet activation,SXS regulated the calcium signaling pathway,and XFZYT regulated the PPAR signaling pathway.(2)In the animal experiments,the values of total cholesterol(TC),triglyceride(TG),low density lipoprotein cholesterol(LDL),high density lipoprotein cholesterol(HDL),TC/HDL,and TG/HDL in each group decreased,among which the ones seen in XFZYT,HLXLD,and SXS groups were statistically significant(P<0.05).XFZYT presented the best effect,followed by HLXLD and SXS.XFZYT and HLXLD decreased apolipoprotein B100(apoB100)and increased apolipoprotein A1/apoB100(P<0.05).XFZYT decreased all the values of hematocrit(HCT),plasma viscosity,whole blood viscosity(WBV);HLXLD and SXS affected HCT;and DSY and THSWT regulated WBV(P<0.05).All the five formulas decreased the values of optical density and area of plaque,among which XFZYT and HLXLD showed statistical significance(P<0.05).Conclusion Adjusting fluid shear stress and alleviating the injury of endothelial cells might be the common mechanisms by which the five formulas promote blood circulation and remove blood stasis.Different formulas also have unique targets,which may provide guidance for clinical drug selection.By regulating different indices,the five formulas can regulate blood lipid and hemorheology,improve the state of blood stasis,and decrease the degree of aortic plaque in the blood stasis model rabbits.XFZYT and HLXLD had higher efficacies than DSY,THSWT,and SXS.

万启南辨治内伤发热

万启南教授认为内伤发热不外乎气、血、阴、阳、肝、湿、瘀等,与气血阴阳失衡、脏腑功能失调有关。临证首辨阴阳,再分虚实,辨明气血,归属脏腑;分为阴虚发热、阳虚发热、气虚发热、血虚发热、气郁发热、血瘀发热、痰湿郁热。理气疏肝泻热-加味逍遥散,郁久化火-龙胆泻肝汤,益气养阴助阳-地黄饮子、青蒿鳖甲汤、清骨散、生脉散,清热化湿退热-甘露消毒丹,湿热并重-苍术白虎汤,祛瘀养血退热-血府逐瘀汤、桃红四物汤,清营解毒退热-白虎汤、清营汤、犀角地黄汤、清瘟败毒饮、安宫牛黄丸、紫雪丹。万启南强调辨证施治,攻补兼施,顾护脾胃,辨病与辨证结合。附内伤发热(气血两燔兼气阴两虚)验案1则。

ENDOMETRIOSIS TREATED BY THE METHOD OF RESOLVING BLOOD STASIS TO ELIMINATE OBSTRUCTION IN THE LOWER-JIAO

48 cases of endometriosis were treated with the Neiyi (ectopic endometrium) No. 2 Pills [symbol: see text] 2 [symbol: see text]) composed of fresh Dahuang (Radix et Rhizoma Rhei), Biejia (Carapax Trionycis) and Taoren Shuang (powdered Semen Persicae). After 3 months of treatment, high effective rates were obtained in menorrhalgia, dyspareunia, proctalgia, hysteromyoma, ovary cyst, and tubercles in the pelvic cavity, with a pregnant rate of as high as 26.7% in sterility. Meanwhile, the levels of plasma PGF2 alpha and PGE2 markedly dropped, while that of 6-keto-PGF1 alpha, beta-EP, and HYP significantly elevated.

不同活血化瘀方剂对重型颅脑损伤急性期大鼠的应用风险

目的探讨不同活血化瘀方剂对重型颅脑损伤(s TBI)急性期大鼠的影响。方法 306只SD雄性大鼠随机分为正常组、模型组、脑蛋白水解物组、桃红四物汤、血府逐瘀汤组、通窍活血汤组、补阳还五汤组7组。除正常组外其余各组采用改良的Feeney’自由落体方法制备s TBI大鼠模型。造模成功后脑蛋白水解物组、桃红四物汤组、血府逐瘀汤组、通窍活血汤组、补阳还五汤组分别给予相应药物1. 11 mg/200 g、2. 04 g/200 g、3. 12 g/200 g、1. 92 g/200 g、5. 74 g/200 g灌胃,正常组和模型组给予生理盐水3 ml/200 g灌胃,各组每日均灌胃1次,连续7天。灌胃后随时统计大鼠死亡率,在第1、3、7天分别观察大鼠脑组织病理评分,检测血清微管相关蛋白Tau、胶质纤维酸性蛋白(GFAP)含量。结果实验期间正常组与脑蛋白水解物组大鼠无死亡,其余各组大鼠死亡主要集中在前4天,前4天与正常组比较,模型组、桃红四物汤组、血府逐瘀汤组大鼠死亡率都显著升高(P <0. 01);与模型组比较,桃红四物汤组、血府逐瘀汤组大鼠死亡率也明显升高(P <0. 01),而通窍活血汤组、补阳还五汤组差异无统计学意义(P> 0. 05)。与正常组同时间相比较,各给药组大鼠脑组织病理评分及血清Tau、GFAP水平在3个时间段均明显升高(P <0. 05)。与模型组同时间比较,第1天血府逐瘀汤组、通窍活血汤组和补阳还五汤组大鼠病理评分升高,桃红四物汤组、血府逐瘀汤组、补阳还五汤血清GFAP蛋白水平升高(P <0. 05);而在第3天除桃红四物汤组外,其余各给药组病理评分较模型组降低;脑蛋白水解物组、通窍活血汤组、补阳还五汤血清Tau、GFAP水平降低(P <0. 05);第7天各给药组病理评分及血清Tau、GFAP水平均降低(P <0. 05)。结论 s TBI急性期使用桃红四物汤及血府逐瘀汤会加重病情,增加死亡风险。用活血化瘀药来治疗s TBI急性期的最佳时间段可能在发生损伤第4天后,并且以通窍活血汤和补阳还五汤效果最好。