简介:目的探讨促肝细胞生长素联合1,6-二磷果糖治疗慢性肝炎重度的临床疗效.方法治疗组用促肝细胞生长素120mg,1,6-二磷酸果糖10g静滴,1次/日;对照组用门冬氨酸钾镁30ml,丹参250ml静滴,1次/日.疗程均为4周.结果治疗组明显改善了患者的纳减、恶心、呕吐、腹胀等常见症状,与对照组比较,差异有显著性,P<0.05.治疗组总有效率为96.77%,对照组总有效率为77.42%,两组比较差异有显著性,P<0.05.治疗组TBIL、ALT的下降均较对照组明显,两组比较差异有极显著性,P<0.01.结论促肝细胞生长素联合1,6-二磷酸果糖治疗慢性肝炎重度,有较好的改善临床症状、退黄降酶作用.
简介:瞄准:与ulcerative(UC)在病人的结肠的粘膜检验metalloproteinase-1(MMP-1)和metalloproteinase-1(TIMP-1)的织物禁止者的表示。方法:颠倒抄写聚合酶链反应(RT-PCR),免疫组织化学被用来与UC和控制在病人在mRNA和蛋白质层次学习MMP-1和TIMP-1的表达式。在MMP-1mRNA,TIMP-1mRNA,MMP-1mRNA/TIMP-1mRNA比率和有UC的病人的临床的症状的严厉之间的关系也被分析。结果:MMP-1mRNA和TIMP-1mRNA在的表示溃烂并且煽动了结肠的粘膜在非煽动的结肠的粘膜比那显著地高(P<0.001),但是有不,统计上,在UC病人和正常的非煽动的结肠的粘膜的有效差量控制(P>0.05)。在UC病人的溃烂的结肠的粘膜的MMP-1和TIMP-1的mRNA表达式被80褶层和2.2褶层增加,分别地什么时候与正常控制相比。在煽动的结肠的粘膜,增加分别地是30褶层和1.6褶层。Immunohistochemical分析显示出那在之中溃烂,发炎,并且UC病人的非煽动的结肠的mucosae和正常控制,MMP-1表示的积极的率分别地是87%,87%,40%和35%,并且TIMP-1表示的积极的率分别地是89%,89%,80%和75%。而且,MMP-1mRNA,TIMP-1mRNA和MMP-1mRNA/TIMP-1mRNA比率的表示与临床的症状(P<0.05)的严厉被相关。结论:在结肠的粘膜在UC病人引起细胞外的矩阵(ECM)和溃疡的过多的水解作用的diseased的MMP-1的过多的表示。MMP-1mRNA,TIMP-1mRNA和MMP-1mRNA/TIMP-1mRNA比率能被用作简历标记与UC在病人判定临床的症状的严厉。外长的TIMP-1或MMP-1禁止者治疗是为有UC的病人的新奇治疗。
简介:AIMToinvestigatetherolesandinteractionsofmutThomolog(MTH)-1andhypoxia-induciblefactor(HIF)-1αinhumancolorectalcancer(CRC).METHODS:TheexpressionanddistributionofHIF-1αandMTH-1proteinsweredetectedinhumanCRCtissuesbyimmunohistochemistryandquantitativerealtimepolymerasechainreaction(qRT-PCR).SW480andHT-29cellswereexposedtonormoxiaorhypoxia.ProteinandmRNAlevelsofHIF-1αandMTH-1wereanalyzedbywesternblottingandqRT-PCR,respectively.InordertodeterminetheeffectofHIF-1αontheexpressionofMTH-1andtheamountof8-oxodeoxyguanosinetriphosphate(dGTP)inSW480andHT-29cells,HIF-1αwassilencedwithsmallinterferingRNA(siRNA).GrowthstudieswereconductedoncellswithHIF-1αinhibitionusingaxenografttumormodel.Finally,MTH-1proteinwasdetectedbywesternblottinginvivo.RESULTS:HighMTH-1mRNAexpressionwasdetectedin64.2%ofcases(54/84),andthiswassignificantlycorrelatedwithtumorstage(P=0.023)andsize(P=0.043).HIF-1αproteinexpressionwascorrelatedsignificantlywithMTH-1expression(R=0.640;P〈0.01)inhumanCRCtissues.HypoxicstressinducedmRNAandproteinexpressionofMTH-1inSW480andHT-29cells.InhibitionofHIF-1αbysiRNAdecreasedtheexpressionofMTH-1andledtotheaccumulationof8-oxo-dGTPinSW480andHT-29cells.Intheinvivoxenografttumormodel,expressionofMTH-1wasdecreasedintheHIF-1αsiRNAgroup,andthetumorvolumewasmuchsmallerthanthatinthemocksiRNAgroup.CONCLUSION:MTH-1expressioninCRCcellswasupregulatedviaHIF-1αinresponsetohypoxicstress,emphasizingthecrucialroleofHIF-1α-inducedMTH-1intumorgrowth.
简介:目的观察慢性淤胆型肝炎高压氧治疗前后患者的肝血流、肝功能、肝组织学、超微结构变化。方法随机选择30例住院的慢性淤胆型肝炎患者,用宁波产高压氧纯氧单仓治疗,剂量为2.5MPa,每天2小时,10天为一疗程,休息2天后再行下一疗程,共6个疗程。治疗前后用肝血流图仪和多普勒B超测定肝血流图收缩波和门静脉右支血流量;行肝穿刺活检术,取新鲜肝组织,常规透射电镜病理观察。结果治疗后肝血流图收缩波和肝门静脉右支血流量明显升高;肝功能明显改善;治疗前后二次肝穿活检的10例患者中,9例患者肝组织汇管区淋巴细胞浸润和肝细胞淤胆减轻;8例患者肝细胞线粒体肿胀和Kupffer细胞增生减轻;7例患者肝细胞变性坏死,汇管区炎症、毛细胆管淤胆减轻和溶酶体数量减少;6例患者肝组织内毛细血管增生明显;3例患者肝细胞内内质网增生、间质纤维化程度减轻;2例患者肝细胞内高尔基体扩张、贮脂细胞增生、间质纤维增生减轻。结论高压氧治疗慢性淤胆型肝炎,可增加肝动脉及门静脉右支血流量,改善患者肝脏功能和临床症状,有效地减轻肝细胞和毛细胆管淤胆及肝组织学和超微结构的损伤。
简介:AIM:Toinvestigatetheeffectsofc-mybantisenseRNAoncellproliferationandtheexpressionofc-myb,TGF-β1andα1-Ⅰcollageninculturedhepaticstellatecells(HSC)fromrats.METHODS:Recombinantretroviralvectorofc-mybantisensegene(pDOR-myb)wasconstructed,andthentransfectedintoretroviralpackagecelllinePA317bymeansofDOTAP.ThepseudovirusesproducedfromtheresistantPA317cellswereselectedwithG418toinfectHSCsisolatedfromratlivers.Thecellproliferationwasmeasuredby3-[4,5-Dimethylthiazolzyl]-2,5-diphenyltetrazo-diumbromide(MTT)method.Theexpressionofc-myb,α1-ⅠcollagenandTGF-β1rnRNA,andc-mybproteininHSCswasdetectedwithsemi-quantitivereversetranseription-polymerasechainreaction(RT-PCR)andWestern-blotrespectively.RESULTS:HSCsfromratswereisolatedsuccessfullywiththeviability>98%.InthepDOR-mybinfectedHSCs,thecmybproteinexpression,cellproliferation,andα1-ⅠcollagenandTGF-β1mRNAexpressionwererepressedsignificantlycomparedwiththeircorrespondingcontrolgroups(P<0.01).CONCLUSION:c-mybplaysakeyroleinactivationandproliferationofHSC.c-mybantisenseRNAcaninhibitcellproliferation,α1-ⅠcollagenandTGF-β1mRNAexpression,suggestingthatinhibitionofc-mybgeneexpressionmightbeapotentialwayforthetreatmentofliverfibrosis.