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噬菌体展示的β-淀粉样蛋白表位的免疫原性和治疗效果

Immunogenicity and therapeutic efficacy of phage-displayed beta-amyloid epitopes.

作者信息

Esposito Marianna, Luccarini Ilaria, Cicatiello Valeria, De Falco Diana, Fiorentini Anna, Barba Pasquale, Casamenti Fiorella, Prisco Antonella

机构信息

Istituto di Genetica e Biofisica A. Buzzati Traverso, CNR, Via Pietro Castellino 111, 80131 Naples, Italy.

出版信息

Mol Immunol. 2008 Feb;45(4):1056-62. doi: 10.1016/j.molimm.2007.07.023. Epub 2007 Sep 11.

DOI:10.1016/j.molimm.2007.07.023
PMID:17850871
Abstract

In vitro and in vivo studies indicate that Alzheimer's Disease (AD) could be prevented or treated by active immunization against self-peptide beta-amyloid. In this study, we compared the immunogenicity of different regions of beta-amyloid, displayed on filamentous phages. We established that a filamentous phage displaying epitope 2-6 (AEFRH) of beta-amyloid at the N-terminus of Major Capside Protein (phage fdAD(2-6)) is more immunogenic than a phage displaying epitope 1-7 (DAEFRHD) that differs only in flanking residues. Monthly injections of fdAD(2-6) trigger a robust anti-beta-amyloid antibody response, and afford a significant reduction of plaque pathology in a mouse model of AD, whereas the same treatment, performed with phage fdAD(1-7), induces a lower anti-beta-amyloid titer and does not protect from amyloid deposition. "Memory" anti-amyloid antibodies induced by a single prime-boost cycle with vaccine fdAD(2-6), that have a lower titer compared to antibodies induced by monthly restimulations, do not prevent plaque pathology. Our data show that optimization of epitope display is essential in vaccine design, and suggest that the titer of the anti-amyloid response is the crucial parameter to obtain therapeutic efficacy in vivo.

摘要

体外和体内研究表明,通过针对自身肽β-淀粉样蛋白进行主动免疫,可以预防或治疗阿尔茨海默病(AD)。在本研究中,我们比较了丝状噬菌体展示的β-淀粉样蛋白不同区域的免疫原性。我们确定,在主要衣壳蛋白N端展示β-淀粉样蛋白表位2-6(AEFRH)的丝状噬菌体(噬菌体fdAD(2-6))比仅侧翼残基不同的展示表位1-7(DAEFRHD)的噬菌体具有更强的免疫原性。每月注射fdAD(2-6)可引发强烈的抗β-淀粉样蛋白抗体反应,并在AD小鼠模型中使斑块病理显著减轻,而用噬菌体fdAD(1-7)进行相同处理则诱导较低的抗β-淀粉样蛋白滴度,且不能防止淀粉样蛋白沉积。用疫苗fdAD(2-6)进行单次初免-加强免疫周期诱导的“记忆”抗淀粉样蛋白抗体,其滴度低于每月再次刺激诱导的抗体,不能预防斑块病理。我们的数据表明,表位展示的优化在疫苗设计中至关重要,并表明抗淀粉样蛋白反应的滴度是在体内获得治疗效果的关键参数。

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