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ID:27244694
大小:567.50 KB
页数:39页
时间:2018-12-02
《雷帕霉素对胃癌SGC7901细胞增殖影响及其机制探讨》由会员上传分享,免费在线阅读,更多相关内容在学术论文-天天文库。
1、雷帕霉素对胃癌SGC7901细胞增殖影响及其机制探讨中文摘要目的研究雷帕霉素靶向抑制mTOR信号通路对胃癌SGC7901细胞增殖的影响及其可能机制,为胃癌的药物治疗提供新的思路和方法.方法体外培养胃癌SGC7901细胞,用免疫细胞化学法检测缺氧条件下胃癌SGC7901细胞中mTOR及HIF-1α蛋白表达情况。细胞经不同浓度雷帕霉素分别作用12h、24h、48h、72h,CCK-8法检测雷帕霉素对细胞增殖的抑制作用。半定量RT-PCR检测细胞mT0R和HIF-1αmRNA表达改变情况,WesternBlot法检测细胞mT0R和HIF-1α蛋白表达改变情况。实验所得数据采用SPSS
2、13.0统计分析软件进行处理。结果免疫细胞化学显示,缺氧条件下胃癌SGC7901细胞胞浆中mTOR呈阳性表达,细胞核和细胞浆中HIF-1α均呈阳性表达。雷帕霉素能显著抑制胃癌SGC7901细胞增殖,抑制率随药物浓度和作用时间增加而增加,呈时间-剂量依赖关系。雷帕霉素作用后,细胞mT0R和HIF-1αmRNA及蛋白表达水平均明显下调。结论缺氧条件下,胃癌SGC7901细胞存在mTOR/HIF-1α信号通路的异常活化。在体外雷帕霉素能显著抑制胃癌SGC7901细胞增殖。缺氧条件下,雷帕霉素抑制mTOR/HIF-1α信号通路是其可能机制之一。关键词雷帕霉素胃肿瘤哺乳动物雷帕霉素靶蛋白
3、缺氧诱导因子-1α药物治疗2EffectofRapamycinonhumangastriccarcinomaSGC7901cellsproliferationandapproachofthemechanismsABSTRACTObjectiveToinvestigatetheeffectsofRapamycinoncellproliferationinhumangastriccarcinomaSGC7901cellsandthepotentialmechanismsinvolvedintheinhibitoryeffectsofthemTORsignalingpathway.P
4、rovidethenewideasandoriginalstrategyaboutthedrugtreatmentforhumangastriccarcinoma.MethodsSGC7901cellswereculturedinvitro.TheexpressionofmTORandHIF-1αproteinswasdeterminedbyimmunocytochemicalmethodinSGC7901cellsculturedunderhypoxicconditions.DifferentconcentrationsofRapamycinwereincubatedwith
5、SGC7901cellsfor12hours、24hours、48hoursand72hours.CellproliferationwasmeasuredbyCCK-8assayinRapamycin—treatedSGC7901cells.TheexpressionlevelsofmTORandHIF—lαmRNAwasdetectedbysemi-quantitativeRT-PCR.ThechangeofmTORandHIF—lαproteinswasdeterminedbyWesternBlot.TheexperimentaldatawereprocessedbySPS
6、S13.0.ResultsImmunocytochemistryshowedthatunderhypoxicconditions,mTORwaspositivelyexpressedinthecytoplasmandthatHIF—lαinthenucleusandcytoplasmofSGC7901cells.RapamycincouldsignificantlyinhibittheproliferationofSGC7901cellsinaconcentration-dependentandtime-dependentmanner.Theexpressionlevelsof
7、mTOR、HIF—lαmRNAandmToR、HIF—lαproteinsweresignificantlylowerinRapamycin—treatedSGC7901cellsthanthoseinuntreatedcells.ConclusionsmTOR/HIF—lαsignalingpathwayisabnormallyactivatedinSGC7901cellsunderhypoxicconditions.Rapamycincouldsignificantlyinhibitth
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