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Plexin-B2在人乳腺癌中的表达及临床意义: 2011年; 目的:探讨人乳腺癌中Plexin-B2的表达,以及其与人表皮生长因子受体-2(Her-2)共表达与乳腺癌恶性行为的关系。方法:免疫组化SP法检测15例正常乳腺组织中Plexin-B2蛋白的表达,及112例乳腺癌组织中Plexin-B2和Her-2蛋白的表达。结果:Plexin-B2在癌细胞和正常乳腺组织小叶及导管上皮细胞中的阳性表达率分别为69.64%和60.00%,差异无统计学意义(P>0.05)。Plexin-B2在乳腺癌组织癌周微脉管中的阳性表达率为44.64%,而正常乳腺微脉管均为阴性。癌细胞和癌周微咏管中Plexin-B2的表达正相关(r=0.593,P=0.000),并且都与临床分期及淋巴结转移有关(P<0.05)。Plexin-B2、Her-2共表达比Plexin-B2单阳性的肿瘤临床分期晚、淋巴结转移率高,差异有统计学意义(P<0.05)。结论:Plexin-B2异常表达可能与乳腺癌的恶性进展有关,Plexin-B2-Her-2共表达可能促使乳腺癌的侵袭转移。; 杨丽兰叶双梅阚淳一杨洁蒋学锋马全富吴明富王世宣

人IGF1R启动子克隆及荧光素酶报告基因载体构建: 2014年; 目的克隆人1GF1R基因启动子序列，构建IGF1R基因启动子荧光素酶报告基因载体。方法运用PCR方法从HeLa细胞基因组DNA中获得目的基因；双酶切后连接到荧光素酶报告基因载体上，构建IGF1R基因启动子报告基因载体；将重组质粒转染至HeLa细胞48h后，采用双荧光素酶报告基因系统检测其启动子活性。结果PCR扩增出800bp左右IGF1R基因启动子片段；双酶切及测序鉴定重组体构建正确；转染HeLa细胞后经双荧光素酶报告基因检测确定重组体有启动子活性。结论成功构建了IGF1R启动子报告基因载体，在细胞系中进行初步的活性分析得知所克隆的IGF1R基因调控序列内包含启动子活性区域。; 李莎汪雯雯吴章颖阿比丹·吐尔汗江王世宣; 关键词：IGF1R 启动子荧光素酶报告基因

Quercetin Suppresses HeLa Cells by Blocking PI3K/Akt Pathway被引量：7: 2014年; To explore the effect of quercetin on the proliferation and apoptosis of HeLa cells, HeLa cells were incubated with quercetin at different concentrations. Cell viability was evaluated by MTT assay, cell apoptosis was detected by Annexin- V/PI double labeled cytometry and DNA ladder assay. Cell cycle was flow cytometrically determined and the morphological changes of the cells were ob- served under a fluorescence microscope after Hoechst 33258 staining and the apoptosis-related pro- teins in the HeLa cells were assessed by Western blotting. The results showed that quercetin signifi- cantly inhibited the growth of HeLa cells and induced obvious apoptosis in vitro in a time- and dose-dependent manner. Moreover, quercetin induced apoptosis of HeLa cells in cell cycle-dependent manner because quercetin could induce arrest of HeLa cells at G0/G1 phase. Quercetin treatment down-regulated the expression of the PI3K and p-Akt. In addition, quercetin could down-regulate ex- pression of bcl-2, up-regulate Bax, but exerted no effect on the overall expression of Akt. We are led to conclude that quercetin induces apoptosis via PI3k/Akt pathways, and quercetin has potential to be used as an anti-tumor agent against human cervix oancer.; 项涛方勇王世宣; 关键词：QUERCETIN PI3K P-AKT BAX

SNIP1在宫颈鳞状细胞癌中的表达及意义: 2012年; 目的：探究Smad核内相关蛋白1（Smad nuclear interacting protein 1,SNIP1）在正常宫颈上皮组织及宫颈鳞状细胞癌（宫颈鳞癌）组织中的表达及其意义。方法：免疫组织化学方法及实时荧光定量PCR（Real-time PCR）技术检测SNIP1在23例正常宫颈组织（正常宫颈组）、25例早期宫颈鳞癌组织（Ⅰa~Ⅱa期）（早期宫颈鳞癌组）和45例晚期宫颈鳞癌组织（Ⅱb~Ⅲb期）（晚期宫颈鳞癌组）中的表达。结果：免疫组织化学方法显示SNIP1蛋白在正常宫颈组、早期宫颈鳞癌组及晚期宫颈鳞癌组中胞质强阳性表达率分别为0,36.0%和73.3%;胞核强阳性表达率分别为17.4%,44.0%和71.1%,且三组间胞质与胞核的表达差异均具有统计学意义（P〈0.01）。在伴有淋巴结转移的宫颈鳞癌病例中,SNIP1在胞质、胞核中的强阳性率分别高于不伴淋巴结转移病例,且差异有统计学意义（P〈0.001）。Real-time PCR技术检测显示SNIP1 mRNA在正常宫颈组、早期宫颈鳞癌组及晚期宫颈鳞癌组中表达呈递增趋势,除了正常宫颈组与早期宫颈鳞癌组间差异无统计学意义外,其余各组间差异有统计学意义（P〈0.05）。结论：SNIP1可能参与调控宫颈鳞癌的进展及侵袭转移过程的发生,并有望成为宫颈鳞癌侵袭转移情况的预测因子。; 汪雯雯阿比丹.吐尔汗江王恬栗妍刘丽江王世宣; 关键词：宫颈癌宫颈鳞状细胞癌淋巴结转移

grp78真核表达载体构建及其稳定转染HeLa细胞系建立: 2011年; 目的构建人grp78基因真核表达载体，并建立稳定高表达grp78的人宫颈癌HeLa细胞系。方法用RT—PCR方法从人宫颈癌HeLa细胞中扩增grp78基因编码区，将PCR产物克隆到pcDNA3．1（＋）真核表达载体，构建重组质粒pcDNA3．1（＋）／grp78并测序鉴定。用构建成功的pcDNA3．1（＋）／grp78真核表达载体转染入人宫颈癌HeLa细胞，经G418筛选获得grp78稳定高表达的HeLa细胞系，并用RT—PCR及Western印迹方法鉴定。结果成功构建pcDNA3．1（＋）／grp78真核表达载体，筛选获得稳定高表达人grp78的HeLa细胞系。结论grp78真核表达载体的成功构建和稳定高表达grpTS的HeLa细胞系的建立为进一步研究grp78的功能奠定了基础。; 王恬陶涛杨润峰吴章颖李伟廖书杰王世宣; 关键词：转染

Primary Screening for Breast Diseases among 17618 Women in Wufeng Area, a Region with High Incidence of Cervical Cancer in China被引量：4: 2012年; In this study, the current status for breast diseases in a region with high-incidence of cervical cancer were epidemiologically investigated. From March to August, 2009, 17618 women, from Wufeng area of Hubei province, China, were recruited to screen breast diseases by using breast infrared diagnostic apparatus. Other diagnostic methods, such as B-mode ultrasound, X-ray mammography, needle biopsy and pathological examination were, if necessary, used to further confirm the diagnosis. The screening showed that 5990 of 17618 cases (34.00%) had breast diseases, 5843 (33.16%) had mammary gland hyperplasia, 48 (0.27%) had breast fibroadenoma, 11 (0.06%) had breast carcinoma, and 88 (0.50%) had other breast diseases. The peak morbidity of breast cancer was found in the women aged 50–60 ages. The morbidity of breast cancer was significantly increased in women elder than or equal to 50 years old (n=8, 0.157%) in comparison with that in the subjects younger than 50 years old (n=3, 0.024%) (u=2.327, P<0.05). It was shown that the occurrence of breast diseases was concentrated in women aged 20–40 years, while the total morbidity reached its peak at the age of 30 years and then decreased sharply after age of 40. Compared with the patients elder than or equal to 40 years old (n=3289, 27.46%), the morbidity rate of breast diseases was significantly increased in women less than 40 years old (2648 cases, 47.18%; P<0.001). However, there was no significant difference in the morbidity of breast diseases between the age group of 20–29 years and that of 30–39 years (P=0.453), and both of them were high. There was no significant association between the morbidity of breast diseases and cervical cancer. Since the morbidity of breast diseases was higher among young women, more attention should be paid to the screening of breast diseases among young women for early diagnosis.; 张庆华刘眈黄传英胡婷沈健胡美玲杨茹陈枝岚来主会刘桂玲梅业冬向群英李雄黄科程王少帅潘秀玉严玉婷李夜陈茜奚玲邓东锐汪辉王世宣卢运萍马丁李双; 关键词：SCREENING

Twist介导的衰老逃逸与宫颈癌侵袭转移的关系被引量：1: 2013年; 目的探究Twist介导的衰老逃逸在宫颈癌侵袭转移过程中的作用。方法免疫组织化学法检测70例宫颈鳞状细胞癌标本中Twist和衰老指标CBX3的表达;合成靶向Twist的小干扰RNA瞬时转染宫颈鳞癌细胞SiHa,免疫细胞化学及β-半乳糖苷酶染色检测细胞衰老变化。结果 Twist在早期宫颈鳞癌（Ⅰa~Ⅱa期）及晚期宫颈鳞癌（Ⅱb~Ⅲb期）组织中表达强阳性率分别为6.7%和15.0%,CBX3表达强阳性率分别为10.0%和0%;而在发生或未发生淋巴结转移的宫颈鳞癌组织中,Twist表达强阳性率分别为25.0%和2.4%,CBX3表达强阳性率分别为0%和7.2%。Twist在早、晚期宫颈鳞癌组织表达改变与CBX3相反。低表达Twist的SiHa中CBX3表达上调,并伴有β-半乳糖苷酶染色增强。结论 Twist在宫颈癌发展过程中表达逐渐升高,其介导的衰老逃逸贯穿宫颈癌侵袭转移的整个过程。; 王恬陶涛阿比丹.吐尔汗江汪雯雯栗妍王世宣; 关键词：TWIST 宫颈鳞癌衰老淋巴结转移

人乳头瘤病毒16型E6/E7基因shRNA真核表达载体构建及其对人宫颈癌SiHa细胞增殖及迁移能力的影响被引量：5: 2014年; 目的构建针对人乳头瘤病毒16型E6/E7基因的shRNA真核表达载体,获得稳定表达干扰质粒的人宫颈癌SiHa细胞系并探讨其对SiHa细胞增殖及迁移能力的影响。方法合成3条特异性干扰HPV16 E6/E7基因的shRNA片段并定向插入psilencer 2.1-U6 hygro载体,构建重组质粒psilencer 2.1-U6hygro-shE6/E7并转染入人宫颈癌SiHa细胞,Real-time PCR检测转染后细胞E6/E7 mRNA的表达,选择沉默效应最好的重组质粒并用潮霉素B稳筛,获得稳定表达重组质粒的SiHa细胞,并用real timePCR和Western blot方法进行鉴定;分别运用CCK-8细胞增殖实验和细胞划痕愈合实验检测细胞的增殖及迁移能力。结果测序证实针对HPV16 E6/E7的shRNA真核表达载体psilencer 2.1-U6 hygro-shE6/E7构建正确;转染psilencer 2.1-U6 hygro-shE6/E7的SiHa细胞HPV16 E6/E7表达明显受抑,同时其增殖及迁移能力也明显受抑制。结论 psilencer 2.1-U6 hygro-shE6/E7真核表达载体的成功构建并获得稳定沉默表达HPV16 E6/E7的人宫颈癌SiHa细胞系,证实沉默表达HPV16 E6/E7的SiHa细胞增殖及迁移能力会明显受到抑制,这为进一步研究HPV 16 E6/E7基因在宫颈癌发生发展过程中的功能奠定了实验基础。; 阿比丹.吐尔汗江杨润峰王恬李莎栗妍项涛; 关键词：宫颈癌

卵巢上皮性肿瘤组织中Bub1蛋白的表达及其意义被引量：4: 2011年; 基因组的不稳定性和异倍体细胞的存在是肿瘤细胞的遗传学特征之一，而纺锤体的失控是其重要原因之一。纺锤体检查点，又称有丝分裂检查点，是细胞在长期的进化过程中产生的监控纺锤体形态、染色体着丝点与微管联接及其产生的张力、染色体排列、确保姐妹染色单体精确分离的质控机制。Bubl作为纺锤体检测点蛋白，可能通过染色体不稳定性和非整倍体传代促进肿瘤发生。对于卵巢癌患者，微管稳定剂紫杉醇类药物现已广泛应用于临床，但耐药现象仍频繁出现，相关研究指出，; 吕煊周婷陈刚王世宣; 关键词：卵巢上皮性 BUB1 肿瘤组织染色体不稳定性蛋白

缺氧诱导宫颈癌Siha细胞发生上皮-间叶转化的研究: 2014年; 目的探讨宫颈癌Siha细胞在二氯化钴(CoCl2)诱导的化学缺氧环境中能否发生上皮-间叶转化(EMT),从而获得侵袭性表型,并初步分析其分子机制。方法划痕实验及Transwell体外侵袭实验检测化学缺氧对细胞迁移、侵袭及转移能力的影响;Western blot印迹法、细胞免疫化学及免疫荧光检测缺氧对Siha细胞缺氧诱导因子1α(HIF-lα)、上皮细胞标记分子E-cadherin、间叶细胞标记分子vimentin表达的影响;实时荧光定量聚合酶链反应(qRT-PCR)检测缺氧对EMT诱导因子snail、zeb、twist mRNA表达的影响。结果缺氧可促进人宫颈SCC Siha细胞的迁移、侵袭和转移能力;宫颈癌Siha细胞在常氧、缺氧12 h、缺氧24 h、缺氧48 h条件下E-cadherin蛋白的相对表达逐渐减少,vimentin蛋白的相对表达逐渐增加,缺氧组与常氧组比较差异有统计学意义(P<0.05);缺氧状态下HIF-1α在Siha细胞中聚集,发现Siha细胞形态发生明显变化、且伴有上皮性标记蛋白E-cadherin的表达减弱;Siha细胞twist及snail mRNA的表达与HIF-lαmRNA表达成正相关,且在缺氧12h后差异均有统计学意义(P<0.05)。结论缺氧微环境可能通过活化HIF-lα,调节twist、snail等转录因子的表达,促进宫颈癌细胞发生上皮-间叶转化,产生侵袭性表型。; 袁明高玲邹清靖汪雯雯王世宣; 关键词：缺氧宫颈肿瘤上皮-间叶转化

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