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Epitope mapping of monoclonal antibodies to the paired helical filaments of Alzheimer's disease: identification of phosphorylation sites in tau protein.

机译:阿尔茨海默氏病成对螺旋丝对单克隆抗体的抗原决定簇定位:鉴定tau蛋白中的磷酸化位点。

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摘要

Tau is a neuronal phosphoprotein the expression of which is developmentally regulated. A single tau isoform is expressed in fetal human brain but six isoforms are expressed in adult human brain, with the fetal isoform corresponding to the shortest adult isoform. Phosphorylation is also developmentally regulated, as fetal tau is phosphorylated at more sites than adult tau. In Alzheimer's disease, the six adult tau isoforms become hyperphosphorylated and form the paired helical filament (PHF), the major fibrous component of the neurofibrillary lesions. One way to identify phosphorylated sites in tau is to use antibodies that recognize phosphorylated residues within a specific amino acid sequence. We here characterize the two novel phosphorylation-dependent anti-tau antibodies AT270 and AT180 and identify their epitopes as containing phosphorylated Thr-181 and Thr-231 respectively. With these antibodies we show that these two threonine residues are partially phosphorylated in fetal and adult tau and almost fully phosphorylated in PHF tau. This result contrasts with previous studies of Ser-202 and Ser-396 which are partially phosphorylated in fetal tau, unphosphorylated in adult tau but almost fully phosphorylated in PHF tau.
机译:Tau是一种神经元磷蛋白,其表达受到发育调节。单个tau同工型在胎儿人脑中表达,但是六个同工型在成人人脑中表达,胎儿同工型对应于最短的成人同工型。磷酸化也受到发育调节,因为胎儿tau比成人tau在更多的位置被磷酸化。在阿尔茨海默氏病中,六种成人tau亚型变得高度磷酸化并形成成对的螺旋丝(PHF),这是神经原纤维病变的主要纤维成分。鉴定tau中磷酸化位点的一种方法是使用识别特定氨基酸序列中磷酸化残基的抗体。我们在这里表征两种新型的磷酸化依赖性抗tau抗体AT270和AT180,并确定它们的表位分别包含磷酸化的Thr-181和Thr-231。使用这些抗体,我们显示这两个苏氨酸残基在胎儿和成人tau中被部分磷酸化,在PHF tau中几乎被完全磷酸化。该结果与先前的Ser-202和Ser-396研究相反,后者在胎儿tau中被部分磷酸化,在成年tau中未磷酸化,而在PHF tau中几乎被完全磷酸化。

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