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大鼠热休克蛋白72基因真核表达载体构建及在COS7细胞中的表达     被引量:3

Construction of eukaryotic expression vector carrying rat heat shock protein 72 gene and its expression in COS7 cells

文献类型:期刊文献

中文题名:大鼠热休克蛋白72基因真核表达载体构建及在COS7细胞中的表达

英文题名:Construction of eukaryotic expression vector carrying rat heat shock protein 72 gene and its expression in COS7 cells

作者:晏春根[1];黄丹文[1];任光圆[1];朱冬芳[1]

机构:[1]绍兴文理学院附属医院内科

年份:2011

卷号:15

期号:18

起止页码:3357

中文期刊名:中国组织工程研究与临床康复

外文期刊名:Journal of Clinical Rehabilitative Tissue Engineering Research

收录:CSTPCD、、Scopus、北大核心2008、CSCD_E2011_2012、北大核心、CSCD

基金:浙江省自然科学基金(Y2100961);浙江省科技计划项目(2009C33129)~~

语种:中文

中文关键词:热休克蛋白72;基因表达;COS7细胞;转录;鉴定

中文摘要:背景:体外克隆、表达热休克蛋白,尤其正常时少量或不表达,而应激时大量表达的热休克蛋白72对研究其缺血再灌注损伤中的作用尤为重要。目的:构建热休克蛋白72基因真核表达载体并于COS7细胞内表达,为HSP72蛋白免疫调节功能的研究奠定基础。方法:采用RT-PCR技术从BABL/C大鼠肝细胞中扩增出热休克蛋白72cDNA,经限制性核酸内切酶消化后,插入真核表达载体pcDNA3.1(+)的相应酶切位点,并将重组质粒转染COS7细胞,进行基因表达鉴定。结果与结论:重组质粒插入基因序列检测证实为热休克蛋白72cDNA,并能在COS7细胞稳定表达。成功构建热休克蛋白72真核表达载体,并于COS7细胞中成功转录与表达。

外文摘要:BACKGROUND:In vitro cloning and expression of heat shock proteins (HSP), especially HSP72, is important in the study of ischemia-reperfusion injuries. OBJECTIVE:To construct eukaryotic expression vector carrying HSP72 and study its transient expression in COS7 cells, and to establish the foundation for further research of the immune function of HSP72. METHODS:HSP72 cDNA was amplified from hepatocytes of BABL/C mice by RT-PCR, and correctly inserted into corresponding sites of eukaryotic expression vector pcDNA3.1(+)after restriction endonuclease digestion, and the recombinant plasmid was transfected into COS7 cells and gene expression was determined by RT-PCR. RESULTS AND CONCLUSION:The gene fragment inserted into the vector pcDNA3.1(+)was confirmed by nucleotide sequencing, and the recombinant plasmid mRNA was successfully expressed in COS7 cells.

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