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叶酸/聚酰胺-胺作为miR-7基因载体的胶质瘤靶向性研究
  • ISSN号:1000-8578
  • 期刊名称:肿瘤防治研究
  • 时间:2012.1.1
  • 页码:1-5
  • 分类:R739.41[医药卫生—肿瘤;医药卫生—临床医学]
  • 作者机构:[1]天津市第五中心医院病理科,天津300450, [2]天津医科大学总医院,天津市神经病学研究所,教育部中枢神经系统创伤修复与再生重点实验室,天津市神经损伤变异与再生重点实验室,天津300162, [3]天津市第五中心医院神经外科,天津300450, [4]杜克大学生物医学工程系,北卡罗菜纳州达勒姆27708, [5]天津市第五中心医院中心实验室,天津300450, [6]天津市第五中心医院中医内科,天津300450
  • 相关基金:1.国家自然科学基金资助项目(编号:81000901)2.天津市卫生局科技基金资助项且(编号:2011KZ26,2011KZ24)3.滨海新区卫生局医药卫生科技项目(编号:2011BHKZ(D4)
  • 相关项目:miR-7联合miR-17-5P小RNA干扰片段共同阻遏胶质母细胞瘤G1/S转化的研究
中文摘要:

【摘要】目的:探讨细胞间连接蛋白43(connexin43,CX43)与水通道蛋白4(aquaporin4,AQP4)在联合诱导成胶质细胞瘤性脑水肿形成过程中的功能偶联机制。方法:在大鼠颅内建立C6胶质瘤脑移植模型,磁共振成像检测成瘤及水肿情况,免疫荧光法和蛋白质印迹法检测肿瘤内部及瘤周CX43和AQ的表达特点。体外采用_P4低渗环境培养C6胶质瘤细胞和正常胶质细胞后,反转录PCR法比较2种细胞中CX43和AQP4的mRNA表达变化趋势;采用小干扰RNA(smallinterferenceRNA,siRNA)技术分别沉默C6胶质瘤细胞和正常胶质细胞中AQP4和CX43的表达,检测另一基因的表达变化。结果:C6胶质瘤脑移植模型中,胶质瘤内部CX43表达缺失和AQ_P4表达水平轻度增高,瘤周则表现为CX43表达水平轻度增高和AQ明显高表达。体外实验发现,低渗环境下正常胶质细胞和胶质瘤细胞中和CX43的水平随时_P间4C6AQP4mRNA的延长均有不同程度的升高,但正常胶质细胞的变化程度明显低于肿瘤细胞,且CX43的变化时间窗落后于AQP4。siRNA沉默C6细胞的AQP4表达后,其CX43表达水平的升高程度明显下降(P〈0.05);沉默正常细胞的CX43表达后,其AQ水平则无_P4明显变化(P〉0.05)。结论:AQP4和CX43在胶质瘤内部及其边缘存在2种不同的致脑水肿机制,CX43可能是AQ的潜在下游调控因子。

英文摘要:

Objective: To search for the coupling mechanism of connexin 43 (CX43) and aquaporin 4 (AQP4) together inducing brain edema formation in glioma. Methods: Intracranial C6 glioma xenograft models were established in the rats, then magnetic resonance imaging detection was used to find the tumor and brain edema, and immunofluorescence and Western blotting method were used to detect CX43 and AQP4 expressions in both intratumoral and peritumoral tissues. C6 glioma cells and normal glial cells were cultured in hypotonic medium, then RT-PCR (reverse transcription-PCR) was used to detect andcompare CX43 and AQP4 mRNA expression trends. AQP4 or CX43 expression was silenced in C6 glioma cells and normal glial cells by siRNA (small interference RNA) technology, then the other genetic change was detected by RT-PCR. Results: In C6 glioma xenograft models, CX43 expression was missed and AQP4 expression was slightly elevated in the intratumoral tissues. But in the peritumoral tissues, CX43 expression was slightly elevated and AQP4 expression was significantly increased. In vitro, the hypotonic environment induced elevation of AQP4 and CX43 mRNA levels with time-varying degrees in both normal glial cells and C6 glioma cells, but the change degree of normal glial cells was significantly lower than that of tumor cells, and the time window of CX43 changes was backward of AQP4. The elevated degree of CX43 was significantly decreased when AQP4 expression was silenced by siRNA in C6 cells (P 〈 0.05), while the AQP4 expression was not affected by CX43 expression silencing in normal cells (P 〉 0.05). Conclusion: There are two different mechanisms of AQP4 and CX43 inducing brain edema formation intratumorally and in the edqe of qlioma. CX43 may be one of the potential downstream regulatory factors of AQP4.

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期刊信息
  • 《肿瘤防治研究》
  • 中国科技核心期刊
  • 主管单位:中华人民共和国卫生部
  • 主办单位:湖北省卫生厅 中国抗癌协会 湖北省肿瘤医院
  • 主编:魏少忠
  • 地址:武昌卓刀泉南路116号
  • 邮编:430079
  • 邮箱:zlfzyj@263.net.cn
  • 电话:027-87670126
  • 国际标准刊号:ISSN:1000-8578
  • 国内统一刊号:ISSN:42-1241/R
  • 邮发代号:38-70
  • 获奖情况:
  • 中国学术期刊综合评价数据库来源期刊,中国科学引文数据库来源期刊
  • 国内外数据库收录:
  • 美国化学文摘(网络版),英国农业与生物科学研究中心文摘,波兰哥白尼索引,美国剑桥科学文摘,日本日本科学技术振兴机构数据库,中国中国科技核心期刊,中国北大核心期刊(2004版),中国北大核心期刊(2008版),中国北大核心期刊(2011版),中国北大核心期刊(2014版)
  • 被引量:17449