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免疫融合蛋白sFcεRIα/mIg(IgG2)的研制
引用本文:马金伟,程虹,褚学者,李先钟,扈艳红,喻志爱,林峰,何丽华,白先宏,胡品良.免疫融合蛋白sFcεRIα/mIg(IgG2)的研制[J].中国生物工程杂志,2010,30(10):17-21.
作者姓名:马金伟  程虹  褚学者  李先钟  扈艳红  喻志爱  林峰  何丽华  白先宏  胡品良
作者单位:百泰生物药业有限公司 北京 100176
基金项目:国家"重大新药创制"重大专项(2009ZX09401-005)资助项目
摘    要:哮喘、过敏性鼻炎、特应性皮炎及食物过敏等疾病为一类常见疾病,但存在治疗效果不佳,患者病程长等特点。IgE 分子是导致过敏性疾病的关键分子。抑制IgE分子与效应细胞膜表面FcεRI受体的结合可抑制过敏反应的发生。通过克隆FcεRI受体α亚基的cDNA与IgG2的稳定区铰链区、CH2和CH3的cDNA连接,以二聚化融合蛋白sFcεRIα/mIg(IgG2)的形式在CHO细胞中表达,达到提高sFcεRIα生物半衰期的目的。表达载体构建和初步的功能性试验等一系列研究证实,所表达的融合蛋白的分子量为170kDa,并与人IgE和鼠IgE有较好的结合活性。这些研究为该融合蛋白最终实现产业化打下良好基础。

关 键 词:I  型过敏反应疾病  IgE  sFcεRIα  融合蛋白  
收稿时间:2009-09-29
修稿时间:2010-08-10

Development of Chimera Protein: sFcεRIα/mIg(IgG2)
MA Jin-wei,CHENG Hong,CHU Xue-zhe,LI Xian-zhong,HU Yan-hong,YU Zhi-ai,LIN Feng,HE Li-hua,BAI Xian-hong,HU Pin-liang.Development of Chimera Protein: sFcεRIα/mIg(IgG2)[J].China Biotechnology,2010,30(10):17-21.
Authors:MA Jin-wei  CHENG Hong  CHU Xue-zhe  LI Xian-zhong  HU Yan-hong  YU Zhi-ai  LIN Feng  HE Li-hua  BAI Xian-hong  HU Pin-liang
Institution:Biotech Pharmaceutical Ltd. Beijing 100176,China
Abstract:IgE plays a key role in type I hypersensitivity reactions. The blocks of IgE binding to its high affinity receptor FcεRI can efficiently eliminate allergic reaction. The sFcεRIα/mIg(IgG2)was constructed by gene fusion of the extracellular portion of α subunit of FcεRI receptor with human IgG2 hing region, CH2 and CH3 region. The chimera could be a markedly longer plasma half-life than the soluble extracellular domain. This chimeric protein was produced by transfecting Chinese Hamster Ovary cells (CHO). Following affinity purification, the apparent molecular weight of sFcεRIα/mIg(IgG2), which showed high affinity with human and mouse IgE, was above 170 kDa. A good foundation for industrialization of this new engineered soluble protein for type I hypersensitivity diseases was provided.
Keywords:Type I hypersensitivity diseases IgE sFc&epsilon  RI&alpha  Fusion protein
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