编码表皮生长因子受体Ⅲ型突变体PEP3表位的cDNA的克隆
基因克隆,,表皮生长因子受体Ⅲ型突变体;PEP3表位;cDNA;基因克隆,1材料与方法,2结果,3讨论,参考文献:
作者简介:段小艺(1974),女(汉族),讲师,博士研究生. 研究方向:肿瘤核医学.摘要:目的 克隆出针对表皮生长因子受体Ⅲ型突变体(EGFRvⅢ)PEP3表位的cDNA片段,为高表达EGFRvⅢ肿瘤的免疫治疗奠定基础。方法 根据PEP3的碱基序列设计出有12对互补碱基的正负引物,正负引物互为模板进行PCR扩增,制备出两端含酶切位点的PEP3 cDNA片段,再将扩增的PCR产物亚克隆于载体pGEMT Easy构建重组质粒pGEMT Easy/PEP3。结果 经限制性内切酶酶切鉴定和DNA测序证实,编码PEP3的cDNA片段被成功扩增并亚克隆于载体pGEMT Easy中。结论 成功克隆了编码表皮生长因子受体Ⅲ型突变体PEP3表位的cDNA片段。
关键词:表皮生长因子受体Ⅲ型突变体;PEP3表位;cDNA;基因克隆
Clone of cDNA encoding PEP3 epitope of epidermal growth factor receptor type Ⅲ mutantDuan Xiaoyi, Wang Jiansheng, Guo Youmin, Liu Min,Zhou Bin, Wang Quanying, Yang Guangxiao
(1. Department of Nuclear Medicine;
2. Department of Oncosurgery, First Affiliated Hospital,Medical School of Xian Jiaotong University, Xian 710061;
3. Image Centre, SecondAffiliated Hospital, Medical School of Xian Jiaotong University, Xian 710004;
4. Xian Huaguang Biological Engineering Company, Xian 710025, China)
ABSTRACT: Objective Through cloning the cDNA fragment encoding PEP3 epitope of epidermal growth factor receptor type Ⅲ mutant(EGFRvⅢ) to establish the base for immunotherapy of carcinoma with high EGFRvⅢ expressing. Methods Designing the primer according to the base sequence of PEP3, cDNA was synthesized and amplificated by PCR. Then, the PCR product was subcloned into vector pGEMT Easy so as to construct recombinant plasmid pGEMT Easy/ PEP3. Results Zymocutting restriction enzyme identification and DNA sequencing conformed that cDNA encoding PEP3 was amplified and subcoloned into pGEMT Easy successfully. Conclusion cDNA encoding PEP3 epitope of EGFRvⅢ was coloned successfully. ......
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