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首页> 外文期刊>Scientific reports. >A novel recombinant 6Aβ15-THc-C chimeric vaccine (rCV02) mitigates Alzheimer’s disease-like pathology, cognitive decline and synaptic loss in aged 3?×?Tg-AD mice
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A novel recombinant 6Aβ15-THc-C chimeric vaccine (rCV02) mitigates Alzheimer’s disease-like pathology, cognitive decline and synaptic loss in aged 3?×?Tg-AD mice

机译:一种新型重组6Aβ15-THC-C-C嵌合疫苗(RCV02)减轻了阿尔茨海默病的病理学,认知下降和突触损失在3岁?×tG-AD小鼠中

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Alzheimer's disease (AD) is a neurodegenerative disorder that impairs memory and cognition. Targeting amyloid-β (Aβ) may be currently the most promising immunotherapeutic strategy for AD. In this study, a recombinant chimeric 6Aβ15-THc-C immunogen was formulated with alum adjuvant as a novel Aβ B-cell epitope candidate vaccine (rCV02) for AD. We examined its efficacy in preventing the cognitive deficit and synaptic impairment in 3?×?Tg-AD mice. Using a toxin-derived carrier protein, the rCV02 vaccine elicited robust Aβ-specific antibodies that markedly reduced AD-like pathology and improved behavioral performance in 3?×?Tg-AD mice. Along with the behavioral improvement in aged 3?×?Tg-AD mice, rCV02 significantly decreased calpain activation concurrent with reduced soluble Aβ or oligomeric forms of Aβ, probably by preventing dynamin 1 and PSD-95 degradation. Our data support the hypothesis that reducing Aβ levels in rCV02-immunized AD mice increases the levels of presynaptic dynamin 1 and postsynaptic PSD-95 allowing functional recovery of cognition. In conclusion, this novel and highly immunogenic rCV02 shows promise as a new candidate prophylactic vaccine for AD and may be useful for generating rapid and strong Aβ-specific antibodies in AD patients with pre-existing memory Th cells generated after immunization with conventional tetanus toxoid vaccine.
机译:阿尔茨海默病(AD)是一种损害记忆和认知的神经变性疾病。靶向淀粉样蛋白-β(Aβ)可能是目前广告的最有前途的免疫治疗策略。在该研究中,将重组嵌合6Aβ15-THC-C免疫原配制用alum佐剂作为新的Aβb细胞表位候选疫苗(RCV02)。我们检查了预防3?×tG-AD小鼠中的认知缺陷和突触损伤的疗效。使用毒素衍生的载体蛋白质,RCV02疫苗引发了稳健的Aβ特异性抗体,其显着降低了adl样病理和3×β-ad ad小鼠的3〜β-ad-Ad小鼠的行为性能。随着年龄3〜×TG-AD小鼠的行为改善,RCV02显着降低了CALPAIN活化同时,其可溶性Aβ或低聚形式的Aβ,可能是通过预防发动机1和PSD-95降解。我们的数据支持降低RCV02-免疫ad小鼠中的Aβ水平的假设增加了允许功能恢复认知功能恢复的突触动发球1和突触后PSD-95的水平。总之,这种新颖的和高度免疫原性RCV02显示了作为AD的新候选预防疫苗的承诺,可用于在AD患者中产生快速和强烈的Aβ特异性抗体,其在用常规破伤风毒素疫苗免疫后产生的预先存在的记忆TH细胞。

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