基于生物信息学探究NR1H4在慢性萎缩性胃炎及药物预测中的作用

目的通过生物信息学方法获得慢性萎缩性胃炎(chronic atrophic gastritis,CAG)的差异基因,预测治疗CAG的小分子药物。方法通过基因表达综合(Gene Expression Omnibus,GEO)数据库获取2份CAG芯片(GSE27411、GSE116312)基因表达样本,利用R语言筛选出CAG差异表达基因,获得CAG免疫相关基因进行基因本体论(gene ontology,GO)和京都基因与基因组百科全书(Kyoto Encyclopedia of Genes and Genomes,KEGG)分析。利用STRING数据库构建蛋白质-蛋白质相互作用(protein-protein interaction,PPI)网络,筛选出核心基因,进一步研究核心基因的免疫浸润,预测其小分子化合物,通过MOE2022进行分子对接,通过GEPIA2网站进行生存分析。结果基于GEO数据库筛选出差异基因517个。GO富集分析发现主要涉及粒细胞趋化性、白细胞趋化性、中性粒细胞趋化性等生物过程。KEGG富集分析显示主要富集于细胞因子-细胞因子受体相互作用通路、核因子κB信号通路、白细胞介素-17信号通路。PPI网络筛选前6个核心基因即NR1H4、CCK、CCL20、CXCL1、LCN2、SAA1,通过相关验证,NR1H4作为核心基因。免疫细胞浸润分析结果显示中央记忆CD8 T细胞、效应记忆CD4 T细胞、γδT细胞、自然杀伤细胞、中性粒细胞等免疫细胞可能参与CAG的发生发展,而中性粒细胞与NR1H4呈正相关。分子对接显示柯里拉京、豆甾醇、栀子苷、桔皮素、鹅去氧胆酸、表没食子儿茶素-3-没食子酸酯6种小分子药物与NR1H4有较好的结合力。结论本研究初步探讨CAG的潜在机制,NR1H4作为关键基因与中性粒细胞可能在CAG“炎-癌转化”进程中具有重要意义,可为CAG的“炎–癌转化”机制研究提供一定的参考依据。

游绍伟教授基于“升阳散火法”论治老年性皮肤瘙痒症

老年性皮肤瘙痒症是一种病因复杂且病情反复的难治性皮肤疾病。现代医学对于本病的治疗效果欠佳,难以治愈。游绍伟教授基于李东垣“升阳散火法”理论,从脾胃入手,通过调理脾胃治疗脾胃以外其他系统疾病,抓住脾胃与老年性皮肤瘙痒症的病机联系,从“脾虚、阳郁、阴火”方面进行分析论治,效果显著。

游绍伟运用“通腑法”治疗大肠积滞型腰痛经验

腰痛是指因各种原因导致腰部或气血运行不畅,或失于濡养,引起的以腰部一侧或两侧发生疼痛为主要症状的疾病。中医学认为腰为肾之府,多从肾论治腰痛。游绍伟主任从医20余载,总结多年临证经验,结合古籍经典,基于“脾为之使,胃为之市”理论,认为燥屎积聚肠腑,腰部局部气血运行不畅,也会导致腰痛,并结合胃肠与腰椎的经络、解剖生理、神经调节的关系,运用“通腑法”治疗大肠积滞引起的腰痛疗效较好。本文主要总结游绍伟从脾胃肠论治腰痛的临证经验,并附验案一则,以期为治疗腰痛提供参考。

葛花解酒涤脂汤对酒精性肝病小鼠肝脏组织能量代谢的影响

目的 检测酒精性肝病(ALD)小鼠肝脏组织能量代谢相关指标水平,并探讨葛花解酒涤脂汤的干预作用。方法 40只雄性C57BL/6J小鼠任意分为正常对照组、模型组、葛花解酒涤脂汤高剂量组(4.94 g/kg)、葛花解酒涤脂汤低剂量组(2.47 g/kg)和白藜芦醇组(0.40 g/kg),每组8只。除正常对照组外,其他各组小鼠先予Lieber-DeCarli对照液体饲料喂养5 d,随后予Lieber-DeCarli酒精液体饲料喂养10 d,第16天灌胃31.5%乙醇溶液1次,以制备ALD小鼠模型。造模结束后第2天起,各干预组灌胃相应药物,每日1次,连续9 d。苏木素-伊红染色和油红O染色观察肝脏组织脂肪变性情况;分光光度法检测肝脏组织Na+K+-腺苷三磷酸(ATP)酶、Ca^(2+)Mg^(2+)-ATP酶活性,琥珀酸脱氢酶(SDH)、肝糖原含量;反相高效液相色谱法检测肝脏组织ATP、腺苷二磷酸(ADP)和腺苷一磷酸(AMP)含量,以及AMP/ATP值、总腺苷酸池(TAN)含量、能荷值(EC);实时荧光PCR法检测肝脏组织沉默信息调节因子1(SIRT1)、腺苷酸活化蛋白激酶(AMPK)α2 mRNA表达;蛋白质印迹法检测肝脏组织SIRT1、AMPKα2、AMPKβ1蛋白表达。结果 与正常对照组比较,模型组小鼠肝脏组织脂肪变性病变明显,肝脏组织Ca^(2+)Mg^(2+)-ATP酶活性、SDH含量降低,肝糖原含量升高,EC、AMP/ATP值降低,ATP、ADP、AMP和TAN含量升高,SIRT1、AMPKα2 mRNA表达降低,AMPKβ1蛋白表达升高(均P<0.05)。与模型组比较,葛花解酒涤脂汤高、低剂量组肝脏组织脂肪变性明显减轻,肝脏组织Na+K+-ATP酶活性降低,EC及SIRT1、AMPKα2 mRNA表达升高(均P<0.05);葛花解酒涤脂汤低剂量组Ca^(2+)Mg^(2+)-ATP酶活性、SDH及ATP含量升高(均P<0.05);葛花解酒涤脂汤高剂量组AMP/ATP值升高(P<0.05);葛花解酒涤脂汤高、低剂量组和白藜芦醇组肝脏组织SIRT1蛋白表达升高(均P<0.05);葛花解酒涤脂汤低剂量组和白藜芦醇组AMPKα2蛋白表达升高(均P<0.05)。与葛花解酒涤脂汤高剂量组比较,葛花解酒涤脂汤低剂量组、白藜芦醇组肝脏组织ATP、TAN含量和EC升高,AMP/ATP值降低(均P<0.05);葛花解酒涤脂汤低剂量组AMPKα2 mRNA表达降低(P<0.05);白藜芦醇组SIRT1、AMPKα2蛋白表达升高(均P<0.05)。与葛花解酒涤脂汤低剂量组比较,白藜芦醇组AMPKβ1蛋白表达降低(P<0.05)。结论 慢性酒精摄入引起的能量代谢改变可能与小鼠ALD发生有关,葛花解酒涤脂汤干预可以改善ALD小鼠肝脏能量代谢异常。

Gehua Jiejiu Dizhi decoction(葛花解酒涤脂汤)ameliorates alcoholic fatty liver in mice by regulating lipid and bile acid metabolism and with exertion of antioxidant stress based on 4DLabel-free quantitative proteomic study

OBJECTIVE:To analyze the effect and molecular mechanism of Gehua Jiejiu Dizhi decoction(葛花解酒涤脂汤,GJDD)on alcoholic fatty live disease(AFLD)by using proteomic methods.METHODS:The male C57BL/6J mouse were randomly divided into four groups:control group,model group,GJDD group and resveratrol group.After the AFLD model was successfully prepared by intragastric administration of alcohol once on the basis of the Lieber-DeCarli classical method,the GJDD group and resveratrol group were intragastrically administered with GJDD(4900 mg/kg)and resveratrol(400 mg/kg)respectively,once a day for 9 d.The fat deposition of liver tissue was observed and evaluated by oil red O(ORO)staining.4DLabel-free quantitative proteome method was used to determine and quantify the protein expression in liver tissue of each experimental group.The differentially expressed proteins were screened according to protein expression differential multiples,and then analyzed by Gene ontology classification and Kyoto Encyclopedia of Genes and Genomes pathway enrichment.Finally,expression validation of the differentially co-expressed proteins from control group,model group and GJDD group were verified by targeted proteomics quantification techniques.RESULTS:In semiquantitative analyses of ORO,all kinds of steatosis(ToS,MaS,and MiS)were evaluated higher in AFLD mice compared to those in GJDD or resveratroltreated mice.4DLabel-free proteomics analysis results showed that a total of 4513 proteins were identified,of which 3763 proteins were quantified and 946 differentially expressed proteins were screened.Compared with the control group,145 proteins were up-regulated and 148 proteins were down-regulated in the liver tissue of model group.In addition,compared with the model group,92 proteins were up-regulated and 135 proteins were downregulated in the liver tissue of the GJDD group.15 differentially co-expressed proteins were found between every two groups(model group vs control group,GJDD group vs model group and GJDD group vs control group),which were involved in many biological processes.Among them,11 differentially co-expressed key proteins(Aox3,H1-5,Fabp5,Ces3a,Nudt7,Serpinb1a,Fkbp11,Rpl22l1,Keg1,Acss2 and Slco1a1)were further identified by targeted proteomic quantitative technology and their expression patterns were consistent with the results of 4D label-free proteomic analysis.CONCLUSIONS:Our study provided proteomics-based evidence that GJDD alleviated AFLD by modulating liver protein expression,likely through the modulation of lipid metabolism,bile acid metabolism and with exertion of antioxidant stress.

基于NF-κB信号通路探讨萎胃通调汤对大鼠慢性萎缩性胃炎的作用机制

目的:探析萎胃通调汤对大鼠慢性萎缩性胃炎(CAG)的干预作用及其可能的机制。方法:90只SD大鼠随机分为正常组,模型组,萎胃通调汤高、中、低剂量干预组,胃复春组6组,每组15只,采用N-甲基-N’-硝基-N-亚硝基胍(MNNG)多因素复合造模法制备CAG大鼠模型。经组织病理学检测鉴定模型制备成功后,给药组分别灌胃给予18、9、4.5 g·kg^(-1)·d^(-1)的萎胃通调汤及0.45 g·kg^(-1)·d^(-1)胃复春水溶液,12周后取大鼠胃黏膜组织经苏木素-伊红(HE)染色后,光学显微镜下观察胃黏膜CAG相关病理学表现;采用实时荧光定量聚合酶链式反应(Real-time PCR)、免疫组织化学法(IHC)及蛋白免疫印迹法(Western blot)分别分析大鼠胃黏膜组织核转录因子-κB(NF-κB)信号通路关键指标mRNA及蛋白表达水平。结果:CAG大鼠胃黏膜固有腺体排列和形态极不规则,伴不同程度减少或消失,固有层可见炎性细胞浸润,约48.4%出现肠上皮化生表现。萎胃通调汤处理后显著改善CAG大鼠胃黏膜固有腺体减少与肠化生等病理改变,呈一定的剂量依赖关系。与正常组比较,模型组大鼠胃黏膜组织环氧合酶2(COX-2)、NF-κB p65、白细胞介素(IL)-1α、IL-1β、IL-10、IL-8α、IL-8βmRNA及COX-2、NF-κB p65、IL-10蛋白表达水平显著上调(P<0.01)。萎胃通调汤及胃复春干预后CAG大鼠胃黏膜组织COX-2、NF-κB p65、IL-1α、IL-1β、IL-10、IL-8α、IL-8βmRNA及COX-2、NF-κB p65、IL-10蛋白表达水平显著下调(P<0.01),其中萎胃通调汤高剂量组相应指标表达水平接近正常组。结论:萎胃通调汤能改善甚至逆转CAG大鼠病变胃黏膜,其作用机制可能与萎胃通调汤下调CAG大鼠胃黏膜组织NF-κB信号通路相关指标mRNA及蛋白表达水平有关。

基于“脾虚宛滞”探讨慢性萎缩性胃炎“炎癌转化”与防治思路

胃“炎癌转化”是从胃的相关性炎症发生、发展到胃癌(GC)的一个过程,其具体发病机制目前尚不明确。在我国,GC无论发病率还是死亡率均较高,预后较差,对部分患者的生活质量及身心健康均造成了较大的影响,构建GC的防治体系具有重要的意义。慢性萎缩性胃炎(CAG)是胃“炎癌”链发生、发展及转归的关键环节,现代医学对于CAG的治疗一般以去除病因及改善临床症状为主,这些治疗虽短期疗效较好,但往往缺乏明显的逆转性且易复发。中医药防治从“整体观念”及“辨证论治”出发,并且结合现代医学对“炎癌转化”的认识,对CAG及GC实施个体化防治原则,防治并重是控制胃“炎癌转化”进程的重要举措。基于CAG本虚标实、虚实夹杂的病机关键提出“脾虚宛滞”理论,认为脾虚是“炎癌转化”之根本,宛是“炎癌转化”之重要因素,滞是“炎癌转化”之关键,“脾虚宛滞”与胃“炎癌转化”进程息息相关。治疗上运用“健脾去宛”之法,其目的是健脾以培元,改善胃腑供血及调节机体免疫力;去宛以通滞,减少非可控性炎症的发生,改善炎性微环境,对胃的相关性炎症进行早期干预,控制胃“炎癌转化”进程,阻断、延缓甚至逆转胃黏膜病变,为CAG的临床诊疗及GC的预防提供新的思路。