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广东省自然科学基金(012402)

作品数:3 被引量:16H指数:3
相关作者:陈伟华中唐深顾大勇吕青更多>>
相关机构:深圳市人民医院清华大学更多>>
发文基金:广东省自然科学基金更多>>
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VEGF-specific siRNAs modified with 2′-deoxy effectively suppress VEGF expression and inhibit growth of nasopharyngeal carcinoma xenograft in a mouse model被引量:7
2008年
Vascular endothelial growth factor (VEGF) is up-regulated in the vast majority of human tumors. The up-regulation of VEGF not only plays important roles in tumor angiogenesis, but also provides a target for tumor treatment with small interfering RNA (siRNA) that targets VEGF; however, it is unclear whether a quite high up-regulation of VEGF will affect the efficiency of RNA interference strategies targeting VEGF. A high level expression of VEGF was found in CNE cells from a nasopharyngeal carcinoma cell line. In this study, we investigate whether VEGF-specific siRNAs can effectively suppress VEGF expression in CNE cells, and study the methods for the use of VEGF-specific siRNAs as potential therapeutic agents. CNE cells with high VEGF expression induced by hypoxia were transfected with VEGF-specific siRNAs. The expression of VEGF was effectively suppressed by VEGF-specific siRNAs, measured by ELISA, Western blot analysis and RT-PCR. Furthermore, experiments in nude mice bearing nasopharyngeal carcinoma xenograft were initiated 5 d after injection of CNE cells. VEGF-specific siRNAs were modified with 2′-deoxy, then injected into the tumors, and a liposome-mediated siRNA transfection system and ultrasound exposure were used to help delivery of the siRNAs. Tumor growth was reduced significantly after 3 weeks' treatment. These studies suggest that VEGF-specific siRNAs still can effectively suppress VEGF expression even in tumor cell lines with a relatively high level of VEGF expression, such as CNE, and VEGF-specific siRNAs modified with 2′-deoxy can be used as potential agents for tumor therapy.
CHEN ShanYi1, GAO GuoFeng1, CHEN Wei1, Lü Qing2, TANG Shen2, HUA Zhong2, YE WenBin2, GU DaYong2, WANG ShaYan1 & ZHANG YaOu2 1 Shenzhen People’s Hospital, Clinical Medical College of Jinan University, Shenzhen 518020, China
关键词:GROWTHNASOPHARYNGEAL
血管内皮生长因子RNA干扰效应对鼻咽癌生长的影响被引量:6
2006年
目的研究RNA干扰(RNA interference)效应对人鼻咽癌低分化上皮细胞株CNE血管内皮生长因子(vascular endothelial growth factor,VEGF)基因表达及肿瘤生长的抑制作用。方法体外转录试剂盒合成VEGF siR-NA;荧光素标记试剂盒标记siRNA;脂质体法将siRNA转入CNE细胞株。荧光显微镜下观察siRNA的转染效率;ELISA检测siRNA对VEGF蛋白表达的抑制作用;用VEGF siRNA转染过的CNE细胞注射入裸鼠,监测裸鼠肿瘤的大小,并采用HE染色,光镜下观察VEGF siRNA对肿瘤组织的影响。结果在VEGF siRNA转染后的CNE细胞株,VEGF的表达得到有效地抑制。对鼻咽癌异种移植肿瘤裸鼠内的治疗观察表明,肿瘤生长在治疗3周后显著减少,病理切片HE染色siRNA组肿瘤的坏死灶增多。结论体外转录合成的siRNA能特异有效地下调VEGF基因的表达,提示用2′-脱氧修饰的VEGF特定siRNA能作为一种有效的肿瘤制剂,为抗鼻咽癌基因治疗提供了新的思路。
高国凤王沙燕陈善义唐深陈伟李先明刘明
关键词:鼻咽肿瘤基因沉默双链RNA血管内皮生长因子RNA干扰
VEGF特异的2′-脱氧修饰siRNA能够有效的抑制VEGF的表达和小鼠鼻咽癌异体移植瘤的生长被引量:3
2008年
血管内皮生长因子(vascular endothelial growth factor,VEGF)在肿瘤血管生成中起重要作用,并在多数肿瘤中表达上调,为使用针对VEGF的小干扰RNA(VEGF siRNA)治疗肿瘤提供了重要的作用靶点.然而,不清楚VEGF表达的大幅上调是否会影响VEGF siRNA的干扰效率.本文研究VEGF siRNA能否在VEGF的表达大幅上调的鼻咽癌细胞(CNE)中有效抑制VEGF的表达,并进一步研究VEGF siRNA作为潜在的抗癌制剂的应用方法.为增加siRNA的稳定性,对VEGF siRNA进行了2'-脱氧(2'-deoxy)化学修饰,再将修饰后的VEGF siRNA导入经低氧诱导而高表达VEGF的CNE细胞,30h后用ELISA,Western blot结果分析和RT-PCR等方法鉴定其抑制CNE细胞表达VEGF的效果,结果证明VEGF的表达被明显抑制.用化学修饰的VEGF siRNA治疗裸鼠的鼻咽癌移植瘤,将VEGF siRNA与脂质体混合后,注射到肿瘤局部,然后进行超声照射.每周治疗2次,3周以后处死裸鼠、分离肿瘤并测量瘤重.结果显示上述治疗能明显抑制鼻咽癌移植瘤的生长.
陈善义高国凤陈伟吕青唐深华中叶文彬顾大勇王莎燕张雅鸥
关键词:鼻咽癌移植瘤
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