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缺陷腺病毒载体表达重复10次的Aβ3-10基因疫苗鼻黏膜免疫APPswe, PSEN1dE9转基因小鼠可诱导出Th2型免疫反应
引用本文:郭蓉,CAO YUN PENG,HUANG KUI,JIANG TONG ZI,LI JIAN,LI YU,XING XIAO NA. 缺陷腺病毒载体表达重复10次的Aβ3-10基因疫苗鼻黏膜免疫APPswe, PSEN1dE9转基因小鼠可诱导出Th2型免疫反应[J]. 中国神经再生研究, 2011, 6(26): 2005-2012
作者姓名:郭蓉  CAO YUN PENG  HUANG KUI  JIANG TONG ZI  LI JIAN  LI YU  XING XIAO NA
作者单位:沈阳市红十字会医院,Department of Neurology,the First Affiliated Hospital of China Medical,Department of Neurology, Shenyang Red Cross Hospital, Shenyang 110013,,Department of Neurology,the First Affiliated Hospital of China Medical,Department of Neurology, the First Affiliated Hospital of Liaoning Medical College, Jinzhou, PR China,Department of Neurology,the First Affiliated Hospital of China Medical,Department of Neurology,the First Affiliated Hospital of China Medical
基金项目:国家自然科学基金课题 (基金编号:30471927)
摘    要:Immunotherapy for Alzheimer’s disease (AD) is effective in improving cognitive function in transgenic mouse models of AD. Because the AN1792 [beta-amyloid (Aβ) 1-42] vaccine was halted because of T cell mediated meningoencephalitis, many scientists are searching for a novel vaccine to avoid the T cell mediated immune response caused by the Aβ1-42. Importantly, the time when the immunization is begun can influence the immune effect. In this study, an adenovirus vaccine was constructed containing 10 × Aβ3-10 repeats and gene adjuvant CpG DNA. Transgenic AD mice were immunized intranasally for 3 months. After 10 × Aβ3-10 vaccine immunization, high titers of anti-Aβ42 IgG1 predominant antibodies were induced. In spatial learning ability and probe tests, the 10 × Aβ3-10 immunized mice showed significantly improved memories compared to control mice. The 10 × Aβ3-10 vaccine resulted in a robust Th2 dominant humoral immune response and reduced learning deficits in AD mice. In addition, the 10 × Aβ3-10 vaccine might be more efficient if administered before Aβ aggregation at an early stage in the AD mouse brain. Thus, the adenovirus vector encoding 10 × Aβ3-10 is a promising vaccine for AD.

关 键 词:Alzheimer’s disease  immunotherapy  gene vaccine  amyloid plaque  T cell immunity response  neural regeneration
收稿时间:2011-06-08
修稿时间:2011-06-08

Induced Th2 dominant immune response in APPswe, PSEN1dE9 transgenic mice after nasal immunization with an adenoviral vector encoding 10 tandem repeats of beta-amyloid 3-10
guorong,CAO YUN PENG,HUANG KUI,JIANG TONG ZI,LI JIAN,LI YU and XING XIAO NA. Induced Th2 dominant immune response in APPswe, PSEN1dE9 transgenic mice after nasal immunization with an adenoviral vector encoding 10 tandem repeats of beta-amyloid 3-10[J]. Neural Regeneration Research, 2011, 6(26): 2005-2012
Authors:guorong  CAO YUN PENG  HUANG KUI  JIANG TONG ZI  LI JIAN  LI YU  XING XIAO NA
Affiliation:Shenyang Red Cross Hospital,,,,,,
Abstract:Immunotherapy for Alzheimer's disease (AD) is effective in improving cognitive function in transgenic mouse models of AD. Because the AN1792 [beta-amyloid (Aβ) 1-42] vaccine was halted because of T cell mediated meningoencephalitis, many scientists are searching for a novel vaccine to avoid the T cell mediated immune response caused by the Aβ1-42. Importantly, the time when the immunization is begun can influence the immune effect. In this study, an adenovirus vaccine was constructed containing 10 × Aβ3-10 repeats and gene adjuvant CpG DNA. Transgenic AD mice were immunized intranasally for 3 months. After 10 × Aβ3-10 vaccine immunization, high titers of anti-Aβ42 IgG1 predominant antibodies were induced. In spatial learning ability and probe tests, the 10 × Aβ3-10 immunized mice showed significantly improved memories compared to control mice. The 10 × Aβ3-10 vaccine resulted in a robust Th2 dominant humoral immune response and reduced learning deficits in AD mice. In addition, the 10 × Aβ3-10 vaccine might be more efficient if administered before Aβ aggregation at an early stage in the AD mouse brain. Thus, the adenovirus vector encoding 10 × Aβ3-10 is a promising vaccine for AD.
Keywords:Alzheimer's disease   immunotherapy   gene vaccine   amyloid plaque   T cell immunity response   neural regeneration
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