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基于人源化酵母模型的 Tau 单克隆抗体制备:对 Tau 寡聚化及诊断的影响

Tau monoclonal antibody generation based on humanized yeast models: impact on Tau oligomerization and diagnostics.

作者信息

Rosseels Joëlle, Van den Brande Jeff, Violet Marie, Jacobs Dirk, Grognet Pierre, Lopez Juan, Huvent Isabelle, Caldara Marina, Swinnen Erwin, Papegaey Anthony, Caillierez Raphaëlle, Buée-Scherrer Valerie, Engelborghs Sebastiaan, Lippens Guy, Colin Morvane, Buée Luc, Galas Marie-Christine, Vanmechelen Eugeen, Winderickx Joris

机构信息

From Functional Biology, KU Leuven, Kasteelpark Arenberg 31 Box 2433, 3001 Heverlee, Belgium.

From Functional Biology, KU Leuven, Kasteelpark Arenberg 31 Box 2433, 3001 Heverlee, Belgium, ADx NeuroSciences NV, Technologiepark Zwijnaarde 4, 9052 Ghent, Belgium, Fujirebio Europe, Technologiepark Zwijnaarde 6, 9052 Ghent, Belgium.

出版信息

J Biol Chem. 2015 Feb 13;290(7):4059-74. doi: 10.1074/jbc.M114.627919. Epub 2014 Dec 24.

Abstract

A link between Tau phosphorylation and aggregation has been shown in different models for Alzheimer disease, including yeast. We used human Tau purified from yeast models to generate new monoclonal antibodies, of which three were further characterized. The first antibody, ADx201, binds the Tau proline-rich region independently of the phosphorylation status, whereas the second, ADx215, detects an epitope formed by the Tau N terminus when Tau is not phosphorylated at Tyr(18). For the third antibody, ADx210, the binding site could not be determined because its epitope is probably conformational. All three antibodies stained tangle-like structures in different brain sections of THY-Tau22 transgenic mice and Alzheimer patients, and ADx201 and ADx210 also detected neuritic plaques in the cortex of the patient brains. In hippocampal homogenates from THY-Tau22 mice and cortex homogenates obtained from Alzheimer patients, ADx215 consistently stained specific low order Tau oligomers in diseased brain, which in size correspond to Tau dimers. ADx201 and ADx210 additionally reacted to higher order Tau oligomers and presumed prefibrillar structures in the patient samples. Our data further suggest that formation of the low order Tau oligomers marks an early disease stage that is initiated by Tau phosphorylation at N-terminal sites. Formation of higher order oligomers appears to require additional phosphorylation in the C terminus of Tau. When used to assess Tau levels in human cerebrospinal fluid, the antibodies permitted us to discriminate patients with Alzheimer disease or other dementia like vascular dementia, indicative that these antibodies hold promising diagnostic potential.

摘要

在包括酵母在内的不同阿尔茨海默病模型中,已证实 Tau 蛋白磷酸化与聚集之间存在联系。我们利用从酵母模型中纯化出的人 Tau 蛋白制备了新的单克隆抗体,并对其中三种抗体进行了进一步表征。第一种抗体 ADx201 独立于磷酸化状态结合 Tau 富含脯氨酸的区域,而第二种抗体 ADx215 在 Tau 的 Tyr(18) 未磷酸化时检测由 Tau N 端形成的表位。对于第三种抗体 ADx210,由于其表位可能是构象性的,因此无法确定其结合位点。这三种抗体均在 THY-Tau22 转基因小鼠和阿尔茨海默病患者的不同脑切片中染出缠结样结构,并且 ADx201 和 ADx210 还在患者脑皮质中检测到神经炎性斑块。在 THY-Tau22 小鼠的海马匀浆和阿尔茨海默病患者的皮质匀浆中,ADx215 始终能染出患病脑中特定的低聚 Tau 寡聚体,其大小相当于 Tau 二聚体。ADx201 和 ADx210 还能与患者样本中的高阶 Tau 寡聚体及假定的原纤维前体结构发生反应。我们的数据进一步表明,低聚 Tau 寡聚体的形成标志着由 Tau 在 N 端位点磷酸化引发的疾病早期阶段。高阶寡聚体的形成似乎需要 Tau 的 C 端进行额外的磷酸化。当用于评估人脑脊液中的 Tau 水平时,这些抗体使我们能够区分阿尔茨海默病患者或其他痴呆(如血管性痴呆)患者,这表明这些抗体具有良好的诊断潜力。

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