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抗淀粉样β蛋白抗体的交叉反应是否会混淆阿尔茨海默病的研究?

Do anti-amyloid beta protein antibody cross reactivities confound Alzheimer disease research?

作者信息

Hunter Sally, Brayne Carol

机构信息

Department of Public Health and Primary Care, Institute of Public Health Forvie Site, University of Cambridge School of Clinical Medicine, Box 113 Cambridge Biomedical Campus, Cambridge, CB2 0SP, UK.

出版信息

J Negat Results Biomed. 2017 Jan 26;16(1):1. doi: 10.1186/s12952-017-0066-3.

Abstract

BACKGROUND

Alzheimer disease (AD) research has focussed mainly on the amyloid beta protein (Aβ). However, many Aβ-and P3-type peptides derived from the amyloid precursor protein (APP) and peptides thought to derive from Aβ catabolism share sequence homology. Additionally, conformations can change dependent on aggregation state and solubility leading to significant uncertainty relating to interpretations of immunoreactivity with antibodies raised against Aβ. We review evidence relating to the reactivities of commonly used antibodies including 6F3D, 6E10 and 4G8 and evaluate their reactivity profiles with respect to AD diagnosis and research.

RESULTS

Antibody cross-reactivities between Aβ-type, P3-type and Aβ-catabolic peptides confound interpretations of immunoreactivity. More than one antibody is required to adequately characterise Aβ. The relationships between anti-Aβ immunoreactivity, neuropathology and proposed APP cleavages are unclear.

CONCLUSIONS

We find that the concept of Aβ lacks clarity as a specific entity. Anti-Aβ antibody cross-reactivities lead to significant uncertainty in our understanding of the APP proteolytic system and its role in AD with profound implications for current research and therapeutic strategies.

摘要

背景

阿尔茨海默病(AD)研究主要集中在β-淀粉样蛋白(Aβ)上。然而,许多源自淀粉样前体蛋白(APP)的Aβ和P3型肽以及被认为源自Aβ分解代谢的肽具有序列同源性。此外,构象可根据聚集状态和溶解度而改变,这导致与针对Aβ产生的抗体的免疫反应性解释相关的重大不确定性。我们综述了与常用抗体(包括6F3D、6E10和4G8)反应性相关的证据,并评估了它们在AD诊断和研究方面的反应性特征。

结果

Aβ型、P3型和Aβ分解代谢肽之间的抗体交叉反应性混淆了免疫反应性的解释。需要一种以上的抗体才能充分表征Aβ。抗Aβ免疫反应性、神经病理学和假定的APP裂解之间的关系尚不清楚。

结论

我们发现,Aβ作为一个特定实体的概念缺乏清晰度。抗Aβ抗体的交叉反应性导致我们对APP蛋白水解系统及其在AD中的作用的理解存在重大不确定性,对当前的研究和治疗策略具有深远影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3450/5270220/acdfc4329c6b/12952_2017_66_Fig1_HTML.jpg

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