程良斌治疗胆汁淤积性肝病相关瘙痒症的临床经验

现代医学对胆汁淤积性肝病诊疗方案日趋成熟,但对其并发症即胆汁淤积性肝病相关瘙痒症还在探索中,由于缺少特效药物治疗,胆汁淤积性肝病相关瘙痒症临床收效欠佳。程良斌教授长期从事中西医结合肝病治疗工作,在治疗中总结经验,认为胆汁淤积性肝病相关瘙痒症病因包括血热生风、湿热相搏、血虚风燥和瘀血阻络,主要病机为气血失和、生风化燥。治疗中程教授采用内外同治法,内治主张分期论治,强调化瘀祛风的重要性;同时善用解郁安神法改善患者因瘙痒导致的焦虑、失眠等精神类问题。外治则采用中药熏洗,根据瘙痒不同症状及体征临证选方,取得较好的临床疗效。

基于中药网络药理学研究青黛防治原发性胆汁性肝硬化的成分与作用机制

目的:基于中药网络药理学研究青黛防治原发性胆汁性肝硬化(PBC)的主要活性成分与作用靶点,探讨其“多成分-多靶点-多通路”的作用机制。方法:通过GeneCards数据库、人类孟德尔遗传数据库(OMIM)数据库收集PBC治疗靶点;根据中药系统药理学技术平台(TCMSP)构建青黛的化学成分及靶蛋白;找到青黛与PBC的靶蛋白交集,构成Venn图;采用Cytoscape 3.7.1软件构建青黛的“成分-靶点-通路”网络;运用string数据库绘制蛋白互作网络(PPI network);通过R和Bioconductor软件对虚拟筛选到的关键靶蛋白进行GO和KEGG富集分析。结果:从青黛中筛选出8个化合物,这些有效成分可能通过调节NOS2、PTGS2、PTGS1、RXRA等32个潜在靶蛋白,影响核受体活性、类固醇受体活性等69种功能机制而发挥防治PBC作用,涉及人巨细胞病毒感染,IL-17信号通路等109条通路。结论:青黛中靛甙、异靛蓝、靛玉红等活性成分可能是防治PBC的物质基础,其作用机制涉及感染、细胞凋亡等。

机体微环境失调在原发性胆汁性胆管炎发病机制中的作用

原发性胆汁性胆管炎(PBC)是一种慢性进展性自身免疫病,其主要病理表现为肝内胆汁淤积,胆管上皮细胞炎症损伤及肝内中、小胆管的持续性炎症损伤,最终导致肝细胞发生不可逆损伤。PBC的发病机制包括遗传、汇管区炎症损伤、黏膜免疫失调和胆管上皮细胞功能改变,肝脏和机体整体的微环境失调是诱发肝纤维化和肝硬化的始动因素。该文就机体代谢微环境、炎症反应微环境和免疫微环境失调在PBC发病机制中作用的研究进展作一综述。

论智能手机技术的社会性

智能手机技术是关于智能手机研发、生产、销售和使用的活动,具有主体性、意向性、移动性、多功能性和所有权让渡的不完全性等特征。智能手机技术的社会性是指在上述活动中所反映出来的人与人关系的属性。智能手机技术的主体性和移动性延伸了人的感觉器官、神经系统和大脑,增强了人的感知和思维能力;其移动性和多功能性拓展了人与人交往的时空边界,提高了工作效率,增添了生活情趣;其所有权让渡的不完全性决定了其独特的多元主体性,展现了人与人关系的复杂性。智能手机技术的社会性通过渗透于其运行的各个环节而生成,具体表现为国家性、经济性和观念导向性等。

Daifan San intervenes in forkhead box P3 and the interleukin(IL)-23/IL-17A signaling pathway to help prevent and treat primary biliary cirrhosis

OBJECTIVE:To investigate the mechanism by which Daifan San(DFS)prevents and treats primary biliary cirrhosis(PBC)via the forkhead box P3(FoxP3)and interleukin(IL)-23/IL-17A signaling pathways.METHODS:Ninety C57BL/6 mice were randomly divided into the control,model,DFS low-dose,DFS middle-dose,DFS high-dose and ursodeoxycholic acid(UDCA)groups(n=15 per group).A mouse model of PBC was induced using polyinosinic polycytidylic acids(poly I:C).Lymphocyte subset expression in the peripheral blood was analyzed via flow cytometry.The inflammatory cytokines and antimitochondrial autoantibody(AMA)levels were detected via enzyme-linked immunosorbent assays.The expressions and location of typeⅠcollagen,typeⅢcollagen,cytokeratin 19 and FoxP3 in the liver tissue were evaluated via immunohistochemistry.FoxP3,IL-23 and IL-17 expressions in the peripheral blood and liver tissue were evaluated via real-time polymerase chain reaction and western blotting.RESULTS:IL-17,IL-23,IL-8,IL-33,TNF-α,and AMA expressions were significantly increased in the model group and decreased in the DFS and UDCA groups.Conversely,Treg cell and FoxP3 expressions were significantly decreased in the model group and increased in the DFS and UDCA groups.The IL-23/IL-17A signaling pathway was closely correlated with chronic inflammation of the bile duct in PBC and functional deletion of Treg cells,leading to reduced FoxP3 levels and mediating the loss of tolerance in PBC.CONCLUSION:DFS may delay the occurrence and relieve the symptoms of PBC by downregulating IL-23/IL-17A signaling pathway expression and upregulating FoxP3 expression.