miR-200c在子宫内膜癌组织中的表达及与ZEB2蛋白的相关性

目的:探讨miR-200c在子宫内膜癌组织中的表达及与ZEB2的相关性。方法:选取113例子宫内膜癌组织和癌旁组织标本,40例正常子宫内膜癌组织作为对照组,检测组织中miR-200c表达量,以及ZEB2基因和蛋白表达量,利用反义寡核苷酸技术抑制子宫内膜癌RL95-2细胞株中miR-200c表达,检测其对细胞侵袭力的影响,以及细胞中ZEB2基因和蛋白表达。结果:子宫内膜癌组织中miR-200c表达量、ZEB2基因和蛋白表达量均高于癌旁组织和对照组(P<0.05);反义miR-200c转染组穿膜细胞数少于阴性对照组和脂质体组(P<0.05);反义miR-200c转染组细胞中ZEB2基因和蛋白表达量均低于阴性对照组和脂质体组(P<0.05)。结论 :miR-200c在子宫内膜癌组织中呈高表达,可能是通过调控ZEB2而促进肿瘤细胞的浸润和转移。

miR-200b在肝癌中靶向调控Bmi1基因的实验研究

目的研究miR-200b在肝癌中对Bmi1的调控作用,并分析其结合位点。方法首先利用生物信息学软件预测人Bmi1 3′-UTR上mi R-200b可能的结合位点;然后构建Bmi1 3′-UTR野生型和突变型报告载体,应用双荧光素酶报告基因分析检测Bmi1 3′-UTR上mi R-200b的结合位点;最后利用real time PCR和Western blot在人肝癌细胞Hep G2中验证mi R-200b对Bmi1的调控作用。结果人Bmi1 3′-UTR上存在3个mi R-200b的潜在结合位点;双荧光素酶报告基因分析提示,转染mi R-200b-3p mimic后野生型组荧光素酶活性明显低于突变型组;real time PCR和Western blot结果提示在Hep G2细胞中过表达mi R-200b可明显下调Bmi1的表达。结论 mi R-200b在肝癌中可通过靶向结合Bmi1基因3′-UTR特异性调控Bmi1基因的表达。

Micro RNA-320 family is downregulated in colorectal adenoma and affects tumor proliferation by targeting CDK6

AIM: To investigate the microR NA(miR NA) expression during histological progression from colorectal normal mucosa through adenoma to carcinoma within a lesion. METHODS: Using microarray, the sequential changes in miR NA expression profiles were compared in colonic lesions from matched samples; histologically, nonneoplastic mucosa, adenoma, and submucosal invasive carcinoma were microdissected from a tissue sample. Cell proliferation assay was performed to observe the effect of miR NA, and its target genes were predicted using bioinformatics approaches and the expression profile of SW480 transfected with the miR NA mimics. mR NA and protein levels of the target gene in colon cancer cell lines with a mimic control or miR NA mimics were measured using qR TPCR and Western blotting. The expression levels of miR NA and target gene in colorectal tissue samples were also measured.RESULTS: Microarray analysis identified that the miR-320 family, including miR-320 a, miR-320 b, miR-320 c, miR-320 d and miR-320 e, were differentially expressed in adenomaand submucosal invasive carcinoma. The mi R-320 family, which inhibits cell proliferation, is frequently downregulated in colorectal adenoma and submucosal invasive carcinoma tissues. Seven genes including CDK6 were identified to be common in the results of gene expression array and bioinformatics analyses performed to find the target gene of the miR-320 family. We confirmed that mR NA and protein levels of CDK6 were significantly suppressed in colon cancer cell lines with miR-320 family mimics. CDK6 expression was found to increase from non-neoplastic mucosa through adenoma to submucosal invasive carcinoma tissues and showed an inverse correlation with miR-320 family expression.CONCLUSION: MiR-320 family affects colorectal tumor proliferation by targeting CDK6, plays important role in its growth, and is considered to be a biomarker for its early detection.

上皮源性卵巢癌中4种miRNAs的表达及其临床意义

目的 分析上皮源性卵巢癌（EOC）组织中mi R-200a、mi R-141、mi R-205和mi R-34a的表达及其临床意义。方法 44例EOC患者按FIGO分期分为FIGOⅠ~Ⅱ（FIGO早期组）组15例和FIGOⅢ~Ⅳ（FIGO晚期组）组29例,用实时荧光定量PCR定量比较2组4种mi RNAs的表达差异并考察4种mi RNAs表达间的关联。以各组mi RNAs表达的中位数将EOC患者分为mi RNA高表达组和低表达组,比较2组患者间的生存差异。按年龄、FIGO分期、术后是否有残余瘤及术后化疗情况分组,进行Kaplan-Meier生存分析和Cox多因素分析。结果 FIGO晚期组mi R-141的表达高于早期组（P=0.036）。mi R-141的表达与mi R-200a、mi R-205呈正相关,与mi R-34a呈负相关（均P〈0.05）;mi R-200a与mi R-205的表达呈正相关（P〈0.05）。生存分析显示,mi R-200a的表达低,卵巢癌患者无进展生存期短（P=0.035）,FIGO早期组生存率高于FIGO晚期组（P〈0.05）。mi R-200a的表达水平、FIGO分期以及年龄与卵巢癌患者总生存期和无进展生存期有关,mi R-141、mi R-205和mi R-34a的表达水平、术后残余瘤以及化疗与患者生存无关。结论 mi R-200a的表达与卵巢癌患者预后有关,可能是卵巢癌患者预后预测的独立影响指标。

片仔癀上调miR-200a抑制大肠癌耐药细胞转移的作用机制

目的:研究片仔癀对大肠癌耐药细胞转移的影响和对mi R-200a及其靶基因E盒结合锌指蛋白ZEB1/2和下游转移相关基因表达的调控作用。方法:MTT法检测不同浓度5-氟尿嘧啶(5-FU)对HCT-8/5-FU细胞和HCT-8细胞活力的影响;采用黏附实验和Transwell法检测细胞黏附、迁移和侵袭能力的改变;通过Q-PCR检测片仔癀对HCT-8/5-FU细胞mi R-200a的表达;采用免疫荧光检测mi R-200a靶基因ZEB1和ZEB2及其下游E-cadherin、N-cadherin的表达。结果:MTT检测结果显示不同浓度的5-FU干预可显著降低HCT-8细胞活力,对HCT-8/5-FU细胞活力影响较小;片仔癀干预显著降低HCT-8/5-FU细胞黏附、迁移和侵袭能力;可显著上调mi R-200a的表达和E-cadherin的表达,下调ZEB1、ZEB2和N-cadherin的表达。结论:片仔癀干预显著抑制大肠癌耐药细胞的转移,且通过调控mi R-200a/ZEB1/2通路及其下游E-cadherin、N-cadhrin的表达可能是其抑制大肠癌转移的重要内在机制。

miR-200家族——一类新的结直肠癌相关基因

结直肠癌是常见消化道恶性肿瘤,其发病率位居胃肠道肿瘤前列。病人早期无明显症状或不适,缺乏有利的患病指征。目前结直肠癌的治疗仍是以手术切除为主,放射治疗、化疗治疗为辅,据临床实践显示,中西医结合治疗药也能达到一定的治疗效果。但是,纵观患者的总体治愈率和生存率,临床治疗并未能大大改善当前的窘境。为此,对结直肠癌的研究日益受到重视,近年来的研究已深入分子水平,发现某些基因与结直肠癌的演变、预后、治疗等存在联系。数据显示mi R-200家族在结直肠癌中的表达异常,会影响患者的生存率和存活时间,介导肿瘤细胞的恶性生物学行为。并且mi R-200家族能调控上皮-间充质转化（epithelial mesen-chymal transition,EMT）关涉因子,如ZEB1、ZEB2,被认为是EMT相关家族,其在结直肠癌侵袭、转移中的作用亦是当前的研究热点。本研究就mi R-200家族与结直肠癌的联系予以综述,为结直肠癌的进一步研究和临床治疗探讨提供思路。