Department of Molecular Psychiatry and Alzheimer, Graduate School, University Medicine Goettingen, 37075 Goettingen, Germany.
J Biol Chem. 2010 Dec 31;285(53):41517-24. doi: 10.1074/jbc.M110.178707. Epub 2010 Oct 22.
N-terminally truncated Aβ peptides starting with pyroglutamate (AβpE3) represent a major fraction of all Aβ peptides in the brain of Alzheimer disease (AD) patients. AβpE3 has a higher aggregation propensity and stability and shows increased toxicity compared with full-length Aβ. In the present work, we generated a novel monoclonal antibody (9D5) that selectively recognizes oligomeric assemblies of AβpE3 and studied the potential involvement of oligomeric AβpE3 in vivo using transgenic mouse models as well as human brains from sporadic and familial AD cases. 9D5 showed an unusual staining pattern with almost nondetectable plaques in sporadic AD patients and non-demented controls. Interestingly, in sporadic and familial AD cases prominent intraneuronal and blood vessel staining was observed. Using a novel sandwich ELISA significantly decreased levels of oligomers in plasma samples from patients with AD compared with healthy controls were identified. Moreover, passive immunization of 5XFAD mice with 9D5 significantly reduced overall Aβ plaque load and AβpE3 levels, and normalized behavioral deficits. These data indicate that 9D5 is a therapeutically and diagnostically effective monoclonal antibody targeting low molecular weight AβpE3 oligomers.
N-端截短的焦谷氨酸化 Aβ 肽(AβpE3)代表阿尔茨海默病(AD)患者大脑中所有 Aβ 肽的主要部分。与全长 Aβ 相比,AβpE3 具有更高的聚集倾向和稳定性,并且显示出增加的毒性。在本工作中,我们生成了一种新型单克隆抗体(9D5),该抗体选择性地识别 AβpE3 的寡聚体组装,并使用转基因小鼠模型以及来自散发性和家族性 AD 病例的人脑研究了寡聚 AβpE3 的潜在体内参与。9D5 表现出一种不寻常的染色模式,在散发性 AD 患者和非痴呆对照组中几乎无法检测到斑块。有趣的是,在散发性和家族性 AD 病例中观察到明显的神经元内和血管内染色。使用新型夹心 ELISA 鉴定出与健康对照组相比,AD 患者血浆样本中的寡聚物水平显著降低。此外,用 9D5 对 5XFAD 小鼠进行被动免疫显著降低了总 Aβ 斑块负荷和 AβpE3 水平,并使行为缺陷正常化。这些数据表明,9D5 是一种针对低分子量 AβpE3 寡聚物的治疗和诊断有效的单克隆抗体。
