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表达双功能融合蛋白(sCAR-EGF)腺病毒载体的构建及其活性检测
引用本文:任鹏康,王丰,李惠明,李宗海,黄倩.表达双功能融合蛋白(sCAR-EGF)腺病毒载体的构建及其活性检测[J].生物工程学报,2006,22(5):713-719.
作者姓名:任鹏康  王丰  李惠明  李宗海  黄倩
作者单位:1. 上海市第一人民医院中心实验室,上海,200080
2. 上海交通大学附属第一人民医院中心实验室,上海,200080
3. 上海交通大学肿瘤研究所癌基因及相关基因研究国家重点实验室,上海,200032
基金项目:国家自然科学基金;国家重点基础研究发展计划(973计划)
摘    要:为了提高腺病毒载体用于基因治疗的靶向性,采用PCR和体外连接的方法构建了柯萨奇病毒-腺病毒受体(Coxsackievirus-AdenovirusReceptor)胞外段sCAR和表皮生长因子(Epidermalgrowthfactor)EGF融合基因,然后将此融合基因插入穿梭质粒pDC315。利用Ad-MAX腺病毒系统,将重组质粒pDC315-sCAR-EGF与腺病毒骨架质粒pBHGloxΔE13cre共同转染AD-293细胞,成功包装出一种复制缺陷型腺病毒Ad5-CMV-sCAR-EGF。经PCR鉴定该病毒含有sCAR-EGF融合基因片段,Westernblotting证实该病毒能表达sCAR-EGF融合蛋白。体外试验证实该病毒感染细胞所产生的融合蛋白能够引导携带报告基因的腺病毒Ad5-CMV-luc高水平感染肿瘤细胞,为高水平表达EGFR的肿瘤的靶向性基因治疗提供了新的手段。

关 键 词:腺病毒  表皮生长因子受体  基因治疗  柯萨奇病毒-腺病毒受体
文章编号:1000-3061(2006)05-0713-07
收稿时间:03 6 2006 12:00AM
修稿时间:05 12 2006 12:00AM

The Construction of Recombinant Adenovirus Expressing Bifunctional Fusion Protein sCAR-EGF and the Detection of its Activity
REN Peng-Kang,WANG Feng,LI Hui-Ming,LI Zong-Hai,HUANG Qian.The Construction of Recombinant Adenovirus Expressing Bifunctional Fusion Protein sCAR-EGF and the Detection of its Activity[J].Chinese Journal of Biotechnology,2006,22(5):713-719.
Authors:REN Peng-Kang  WANG Feng  LI Hui-Ming  LI Zong-Hai  HUANG Qian
Institution:Central Experimental Laboratory, The First People's Hospital, Shanghai, China.
Abstract:To improve the targeting of adenovirus vector for gene therapy, a fusion gene sCAR-EGF, in which epidermal growth factor gene was fused to the 3' end of extracellular Coxsackie virus-adenovirus receptor gene, was constructed and cloned into shuttle plasmid pDC315 to obtain a recombinant plasmid pDC315-sCAR-EGF. With the AdMax system, AD-293 cells were co-transfected with pDC315-sCAR-EGF and adenovirus genomic plasmid pBHGloxdeltaE13cre. Through high efficiency site specific recombination, a replication-defective adenovirus Ad5-CMV-sCAR-EGF was constructed. The recombinant adenovirus was analyzed by PCR and Western blotting, the results indicated that Ad5-CMV-sCAR-EGF contained the fusion gene sCAR-EGF, and the adenovirus infected cells was induced to produce and secrete the fusion protein into the supernatant. We have demonstrated that the fusion protein sCAR-EGF is helpful for elevating the infection efficiency of Ad5-CMV-luc with the reporter gene in vitro, which providing a new approach to the gene therapy for tumors overexpressing EGFR.
Keywords:adenovirus  epidermal growth factor receptor  gene therapy  Coxsackie virus-adenovirus receptor
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