程丑夫论治心力衰竭合并室性早搏经验

程丑夫教授治疗心力衰竭合并室性早搏具有丰富的经验,认为此病的主要原因为心之阳气亏虚,络脉不通,酿生痰瘀之邪;阳气虚衰、心阴不足为此病之本,痰湿瘀滞窍闭为此病之标。急性期宜温阳益气治心衰水肿,兼理气化痰、除瘀开窍平心悸;急性期尤其重视痰浊邪气闭塞胸中气机之病机,认为宜重用理气化痰开窍药。稳定期宜益气养阴与化痰除瘀并用,标本兼治,尤宜温心阳、养心阴基础上,尤宜配伍健脾益气以杜绝生痰之源,配伍行气化痰、化瘀通络药以祛除痰湿深伏心胸之证。

程丑夫论治慢性疲劳综合征经验

总结程丑夫教授从脾胃气虚湿热论治慢性疲劳综合征的经验。程教授认为,疲劳综合征作为一种慢性疾病,与脾、胃病变的产生有着紧密联系。慢性疲劳综合征的病理因素主要为湿、热,两者合而内生,侵犯脏腑,以致气机升降失调,故临床可见气虚湿困证、气虚内热证。程教授临证多采用升阳益胃汤、知柏益气汤、香砂六君子汤加减治疗本病。

基于数据挖掘分析程丑夫治疗冠心病用药规律

目的:分析程丑夫教授治疗冠心病的中医用药规律,总结临床治疗思路,以期对中医治疗本病有所借鉴。方法:收集程丑夫教授2016年4月—2019年8月门诊治疗冠心病有效处方,依托古今医案云平台(v2.1)建立数据库,统计分析挖掘用药规律。结果:共筛选病案212例,其中女102例,男110例,女︰男=1︰1.08,60岁以上127例,临床患者以中老人为主;共涉及中药139味,以温性、辛苦甘味为主,主入肝经、脾胃经,其中法夏使用频次最多为212次;临床以清热化痰、疏肝解郁为主要治法,柴陷丹参饮为其常用方,其核心药由柴胡、党参、黄芩、木香、砂仁、丹参、黄连、半夏、瓜蒌皮组成。结论:程丑夫教授治疗冠心病以和解少阳、清热化痰为基础,同时辅以活血、益气、养阴等法,标本兼治,具有一定的临床指导意义和传承价值。

程丑夫教授辨治气滞血瘀水停型冠心病心力衰竭经验

冠心病心力衰竭属于中医学"胸痹""痰饮""心水"等范畴,程丑夫教授认为部分冠心病心力衰竭的病机为气、血、水三者互结,情志失调是重要原因,血瘀为中心病理环节,水饮内停为必然结果,辨证为气滞血瘀水停证,以调气活血利水为治法,创柴葶丹参饮以治之,取得良效。

程丑夫运用柴胡疏肝散经验举隅

柴胡疏肝散出自《证治准绳》,主要功效疏肝解郁、行气止痛,为疏肝解郁常用方。程丑夫教授认为,肝郁气滞致病广泛:气机郁滞,肝失疏泄则发为郁证;肝郁气滞化火,上扰心神则不寐;肝气郁滞,横逆犯胃,胃失和降则胃痛;肝失条达,气机郁滞,络脉失和则胁痛。虽病名及临床表现不同,但其总病机归属于肝郁气滞。本文结合案例总结程教授运用柴胡疏肝散的临床经验。

基于数据挖掘的程丑夫治疗冠心病的遣方用药规律研究

目的应用数据挖掘的方法分析和总结程丑夫教授治疗冠心病的遣方用药规律,促进名老中医经验的传承与推广。方法收集整理2019年10月至2021年2月程丑夫教授治疗冠心病的门诊处方,经过筛选并按照统一标准处理后,以符合纳入标准的中药处方为基础,建立数据库。运用中医传承辅助平台软件(V2.5)进行数据挖掘,对处方中的中药进行频数分析、关联分析和聚类分析。结果本研究共收集冠心病患者病案281例,剔除不符合纳入要求的病案62例,共纳入219名冠心病患者的有效处方224则,药物127味。其中气郁痰热、瘀阻心脉证209例,气虚痰热、瘀阻心脉证15例。使用频次位居前5的药物有柴胡、黄芩、法半夏、党参、丹参;药性以温、寒、平为主,药味以辛、苦、甘为主,药物归经主要为脾、胃、肺、肝、胆、心经。经关联规则分析得出药对关联规则24条、角药关联规则23条;经核心药物聚类分析得出10个核心组合与10个新处方。结论程丑夫教授治疗冠心病以调气化痰、活血化瘀为核心,痰瘀同治、气血并调、标本兼顾,常用小柴胡汤、小陷胸汤、丹参饮加减治疗冠心病。

程丑夫运用小柴胡汤经验

《伤寒论》中小柴胡汤具有和解少阳之功,方中柴胡一药性苦平,《神农本草经》谓“治心腹去肠胃中结气、饮食积聚、寒热邪气、推陈致新”。小柴胡汤以和解少阳、调节枢利为主旨,现代临床多用于头痛头晕、失眠、以及消化系统疾病等,程丑夫,主任医师,教授,博士生导师,享受国务院特殊津贴专家,国家级名中医。程丑夫教授谴方谨,药简力专,处方体现了“整体”思想,临床经验丰富。善用小柴胡汤治疗中医内科胸痹心痛病、胃脘病、头痛病等病证,均获得良效。该文对程丑夫教授运用“小柴胡汤”的学术经验进行总结探讨,并附应用实例佐证。

程丑夫运用柴胡加葛汤加减治疗项痹经验

柴胡加葛汤具有疏调气机、解肌通络的功效,程丑夫教授依据治痰、治瘀、治郁、治虚4个治则治疗项痹,注重根据患者主症及兼症辨证诊疗,临床效果卓越。该文主要介绍程丑夫教授运用柴胡加葛汤加减治疗项痹的经验。

Efficacy of Jiangzhi Xiaoban tablet(降脂消斑片)on toll-like receptor 4/nuclear factor-kappa B/nod-like receptor protein 3 signaling pathway in mice with atherosclerosis induced by high-fat diet

OBJECTIVE:To study the effect of Jiangzhi Xiaoban tablet(降脂消斑片,JZXB)on toll-like receptor 4(TLR4)/nuclear factor-kappa B(NF-κB)/Nod-like receptor protein 3(NLRP3)signaling pathway expression in atherosclerosis(AS)mice by establishing a mouse model of AS,and to explore its mechanism of prevention and treatment of AS.METHODS:Sixty-four male C57BL/6J mice were randomly divided into two groups,12 in the normal control group and 52 in the model group(MOD).Seven weeks later,two mice in each of the above two groups were randomly sacrificed,and the whole aortic tissue of the mice was taken out for hematoxylin-eosin staining.After successful modeling,50 mice in the modeling group were randomly divided into 5 groups:MOD,atorvastatin group(ATO),low-dose group of JZXB(JZXB-L),middle-dose group of JZXB(JZXB-M),and high-dose group of JZXB(JZXB-H),10 mice in each group.The mice in each group were killed after 6 weeks of preventive administration.HE staining was used to observe the pathological changes of aorta in AS mice.The levels of serum triglyceride(TG),total cholesterol(TC),low-density lipoprotein cholesterol(LDL-C)and high-density lipoprotein cholesterol(HDL-C)were detected by automatic biochemical analyzer.The levels of inflammatory factor interleukin-1β(IL-1β)were detected by enzyme linked immunosorbent assay.The expression of TLR4,NF-κB and NLRP3 proteins in aortic tissue was detected by immunohistochemistry.RESULTS:Compared with the MOD,the levels of serum TC,TG and LDL-C in the JZXB-H and ATO were significantly decreased,while the level of HDL-C was significantly increased.The levels of serum TG,LDL-C in the JZXB-M were significantly decreased,and the level of HDL-C was significantly increased.Compared with the MOD,the levels of IL-1βwere significantly decreased,aortic lesions were significantly improved,and the expression of TLR4,NF-κB,and NLRP3 proteins in the aortic tissue was significantly decreased in the JZXB-H,JZXB-M,and ATO.CONCLUSION:JZXB has inhibitory effect on atherosclerosis in mice,and its mechanism may be through regulating the TLR4/NF-κB/NLRP3 signaling pathway and reducing the inflammatory response,so as to play a role in inhibiting atherosclerosis.