简介:AIM:Toevaluatetheefficacyofthe14-dmoxifloxacinbasedtripletherapyforthesecond-lineeradicationofHelicobacterpylori(H.pylori)infection.METHODS:Between2011and2013,weconductedaretrospectivereviewofthemedicalrecordsof160patientswhohadexperiencedfailureoftheirfirst-lineprotonpumpinhibitor-basederadicationtherapyandsubsequentlyreceivedthemoxifloxacin-basedtripletherapyasasecond-lineeradicationtreatmentregimen.Thepatientswhoweretreatedwiththemoxifloxacinbasedtripletherapy(oral20mgrabeprazoleb.i.d.,1000mgamoxicillinb.i.d.,and400mgmoxifloxacinq.d.)for7dwereassignedtotheRAM-7group(n=79)whilethosewhotookthemfor14dayswereassignedtoRAM-14group(n=81).Theeradicationratesforbothgroupsweredeterminedbyintentionto-treat(ITT)andper-protocol(PP)analyses.ITTanalysiscomparedthetreatmentgroupsasoriginallyallocatedwhilethePPanalysisincludingonlythosepatientswhohadcompletedthetreatmentasoriginallyallocated.SuccessfuleradicationtherapyforH.pyloriinfectionwasdefinedasthedocumentationofanegative13C-ureabreathtest4wkaftertheendoftheeradicationtreatment.RESULTS:TheoverallITTeradicationratewas76.2%(122/160).ThefinalITTeradicationrateswere70.8%(56/79;95%CI:63.3%-77.1%)intheRAM-7groupand81.4%(66/81;95%CI:74.6%-88.3%)intheRAM-14group(P=0.034).TheoverallPPeradicationratewas84.1%(122/145),andthefinalPPeradicationrateswere77.7%(56/72;95%CI:70.2%-85.3%)intheRAM-7groupand90.4%(66/73;95%CI:82.8%-98.1%)intheRAM-14group(P=0.017).TheH.pylori-eradicationratesintheRAM-14groupweresignificantlyhighercomparedwiththatoftheRAM-7groupaccordingtoboththeITT(P=0.034)andthePPanalyses(P=0.017).Bothgroupsexhibitedgoodtreatmentcompliance(RAM-7/RAM-14group:100%/100%).Theadverseeventrateswere19.4%(14/72)and20.5%(15/73)intheRAM-7andRAM-14groups,respectively(P=0.441).Adverseeventsoccurredin14
简介:AIM:Toinvestigatetheefficacyofneoadjuvantchemoradiotherapy(NACRT)forresectabilityoflocallyadvancedgastriccancer(LAGC).METHODS:BetweenNovember2007andJanuary2014,29patientswithLAGC(clinicallyT3withdistalesophagusinvasion/T4orbulkyregionalnodemetastasis)thatweretreatedwithNACRTfollowedbyD2gastrectomywereincludedinthisstudy.ResectabilitywasevaluatedwithradiologicandendoscopicexamsbeforeandafterNACRT.Usingthreedimensionalconformalradiotherapy,patientsreceived45Gy,withadailydoseof1.8Gy.Theentiretumorextentandtheregionalmetastaticlymphnodeswereincludedinthegrosstumorvolume.PatientspresentingwitharesectabletumorafterNACRTreceivedatotalorsubtotalgastrectomywithD2dissection.ThepathologictumorresponsewasevaluatedusingJapaneseGastricCancerAssociationhistologicevaluationcriteria.PostoperativemorbiditywasevaluatedusingtheNationalCancerInstitute-CommonTerminologyCriteriaforAdverseEventsversion4.0.Overallsurvival(OS)andprogression-freesurvival(PFS)rateswereestimatedusingaKaplan-Meieranalysisandcomparedusingthelog-ranktest.RESULTS:Allpatientswereassessedasunresectablecases.Twenty-fourpatients(24/29;82.8%)showedLAGConpositronemissiontomography-computedtomography(CT)andcontrast-enhancedCT,whereasfourpatients(4/29;13.8%)withvagueinvasionorabutmenttoanadjacentorganunderwentdiagnosticlaparoscopy.Onepatient(1/29;3.4%),initiallyassessedasaresectablecase,underwentan'openandclosure'afterthetumorwasfoundtobeunresectable.Abutmenttoanadjacentorgan(34.5%)wasthemostcommonreasonforNACRT.TheclinicalresponserateonemonthafterNACRTwas44.8%.AfterNACRT,69%(20/29)ofpatientshadaresectabletumor.Ofthe20patientswitharesectabletumor,18patients(62.1%)underwentaD2gastrectomy.TheR0resectionratewas94.4%andtwopatients(2/18;11.1%)showedacompleteresponse.Themedianfollow-updurationwas13.5mo.Theone-yearOSandPFS
简介:背景:维生素D受体(VDR)属于类固醇激素受体超家族,参与细胞增殖、分化、凋亡以及免疫应答等多种生物学过程,在多种恶性肿瘤中呈低表达。目的:探讨VDR在结直肠癌中的表达及其调控机制。方法:收集2010年2月-2012年12月上海交通大学医学院附属仁济医院收治的结直肠癌患者30例,以免疫组化法检测癌组织和相应癌旁非癌组织标本的VDR表达情况。从基因表达汇编(GEO)数据库中提取224例结直肠癌患者的临床资料,分析其癌组织VDR表达与患者临床病理特征和生存期的关系。采用组蛋白-赖氨酸N-甲基转移酶EZH2-siRNA或5-氮杂胞嘧啶核苷(5-AZA)处理人结肠癌细胞株HCT116和SW620,以实时PCR检测VDR表达水平,以甲基化特异性PCR(MSP)检测VDR启动子区甲基化水平。结果:结直肠癌患者癌组织VDR阳性表达率显著低于癌旁非癌组织(26.7%对70.0%,P〈0.001)。结直肠癌组织VDR表达与肿瘤组织学分期、远处转移、脉管转移、淋巴结转移呈负相关(P〈0.05);VDR高表达者生存期显著长于低表达者(P=0.032)。与转染对照-siRNA相比,HCT116、SW620细胞转染EZH2-siRNA后,EZH2mRNA表达水平和VDR启动子区甲基化水平均显著降低(P〈0.05),VDRmRNA表达水平显著升高(P〈0.05)。5-AZA处理HCT116、SW620细胞后,VDR启动子区甲基化水平较阴性对照组显著降低(P〈0.05),VDRmRNA表达水平显著升高(P〈0.05)。结论:结直肠癌中VDR表达下调且与患者预后呈正相关。VDR在结直肠癌中的转录抑制受组蛋白甲基化和DNA甲基化共同调控。
简介:背景:Gankyrin是一个含锚蛋白重复序列的原癌蛋白,其高表达参与了多种恶性肿瘤的发生、发展进程。目的:探讨下调gankyrin表达对胃癌细胞增殖能力的影响及其可能机制。方法:以携带gankyrinsiRNA的慢病毒载体转染人胃癌细胞株MKN28,分别采用MTT实验、流式细胞术和蛋白质印迹法检测下调gankyrin表达对MKN28细胞增殖、细胞周期分布及其β-catenin/cyclinD1信号通路的影响。结果:慢病毒载体的转染效率在90%以上,转染gankyrinsiRNA后,MKN28细胞gankyrin蛋白表达显著受抑(P<0.01)。与未转染慢病毒和转染对照病毒的细胞相比,转染gankyrinsiRNA的MKN28细胞体外生长于第3天起显著受抑,细胞周期G1期细胞比率增高,S期细胞比率降低,细胞中的β-catenin和cyclinD1表达水平降低,差异均有统计学意义(P<0.01)。结论:下调胃癌细胞中的gankyrin表达可通过抑制β-catenin/cyclinD1信号通路引起细胞周期G1期阻滞和细胞增殖抑制,gankyrin有望成为胃癌靶向治疗的新靶点。
简介:【摘要】目的:探讨在小儿咳嗽变异性哮喘治疗中,布地奈德与孟鲁司特钠联合应用对于缓解咳嗽症状、症状消失时间以及平均治疗时间的作用。方法:选择80名诊断为小儿咳嗽变异性哮喘的患者,随机等分为两组:一组为对照组,仅接受布地奈德治疗;另一组为观察组,接受布地奈德和孟鲁司特钠的联合治疗。比较两组患者治疗效果。结果:观察组治疗有效率高于对照组;经过治疗后,观察组FVC和FEV1与对照组作比较更高;观察组咳嗽缓解和消失以及平均治疗时间与对照组做比较更低,差异显著(P<0.05)。结论:将布地奈德与孟鲁司特钠两种药物共同应用于小儿咳嗽变异性哮喘的治疗中,对提升疗效以及改善肺功能具有正面效用,并有效缩短咳嗽持续时间,从而促进患儿更快地恢复健康。
简介:目的:在IBS-D治疗中联合应用奥替溴铵+双歧杆菌,并分析其疗效以及对炎症因子水平的影响。方法:选取2019年1与-2020年1月,在我院治疗的90例IBS-D患者,采取随机数字表法,将其分为两组。对照组45例,应用双歧杆菌三联活菌片;观察组45例,在此基础上,联合应用奥替溴铵治疗。比较两组患者的临床疗效、炎症因子水平。结果:观察组患者总有效率为95.56%,对照组患者总有效率为82.22%,差异明显(P<0.05);治疗后,观察组患者IL-6、IL-8水平明显低于对照组(P<0.05)。结论:在IBS-D治疗中联合应用奥替溴铵+双歧杆菌能够提高治疗效果,下调炎症因子水平,值得推广。