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An Immunomodulatory Therapeutic Vaccine Targeting Oligomeric Amyloid-β1

表位 免疫学 免疫系统 医学 免疫疗法 肽疫苗 抗体 脑膜脑炎 T细胞 病毒学
作者
Ge Song,Haiqiang Yang,Ning Shen,Phillip Pham,Breanna Brown,Xiaoyang Lin,Yuzhu Hong,Sinu Paul,Jianfeng Cai,Xiaopeng Li,Michael Leon,Marcia N. Gordon,David Morgan,Sai Zhang,Chuanhai Cao
出处
期刊:Journal of Alzheimer's Disease [IOS Press]
卷期号:77 (4): 1639-1653 被引量:10
标识
DOI:10.3233/jad-200413
摘要

Background: Aging is considered the most important risk factor for Alzheimer’s disease (AD). Recent research supports the theory that immunotherapy targeting the “oligomeric” forms of amyloid-β (Aβ) may halt the progression of AD. However, previous clinical trial of the vaccine against Aβ, called AN1792, was suspended due to cases of meningoencephalitis in patients. Objective: To develop a peptide sensitized dendritic cells (DCs) vaccine that would target oligomer Aβ and prevent an autoimmune response. Methods: Double transgenic APPswe/PS1ΔE9 (Tg) and C57BL/6J control mice were used in this study. Cytokine expression profile detection, characterization of antisera, brain GSK-3β, LC3 expression, and spatial working memory testing before and post-vaccination were obtained. Results: Epitope prediction indicated that E22W42 could generate 13 new T cell epitopes which can strengthen immunity in aged subjects and silence several T cell epitopes of the wild type Aβ. The silenced T cell epitope could help avoid the autoimmune response that was seen in some patients of the AN-1792 vaccine. The E22W42 not only helped sensitize bone marrow-derived DCs for the development of an oligomeric Aβ-specific antibody, but also delayed memory impairment in the APP/PS1 mouse model. Most importantly, this E22W42 peptide will not alter the DC’s natural immunomodulatory properties. Conclusion: The E22W42 vaccine is possibly safer for patients with impaired immune systems. Since there is increasing evidence that oligomeric form of Aβ are the toxic species to neurons, the E22W42 antibody’s specificity for these “oligomeric” Aβ species could provide the opportunity to produce some clinical benefits in AD subjects.
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