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Ubiquitin is associated with early truncation of tau protein at aspartic acid 421 during the maturation of neurofibrillary tangles in Alzheimer's disease

机译:泛素与阿尔茨海默氏病神经原纤维缠结成熟期间天冬氨酸421处tau蛋白的早期截断有关

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摘要

Pathological processing of tau protein during the formation and maturation of neurofibrillary tangles (NFTs) includes abnormal phosphorylation, conformational changes and truncation of the C-terminus at aspartic-acid 421 (apoptotic product) and glutamic-acid 391 residues. Abnormal phosphorylation and misfolding may serve as recognition signals for ubiquitin-targeting and proteosomal processing. For this reason, we sought to determine whether ubiquitin-targeting of tau is associated with particular tau modifications that herald specific stages of NFTs maturation in the hippocampus of Alzheimer's disease cases. Using multiple tau antibodies, we found that 30% of the total load of NFTs is ubiquitin-associated. As reported previously ubiquitin immunoreactivity was associated with markers of phosphorylated tau in certain NFTs; however, a strong association was also found between ubiquitin and the earliest known truncation event at aspartic-acid 421. These findings indicate that tau protein in the NFTs may be dually subjected to both apoptotic and proteosomal processing. By contrast ubiquitin immunoreactivity was poorly associated with truncation of tau at glutamic-acid 391, suggesting that this proteolytic event may be independent of proteosomal activity. It would appear, therefore, that ubiquitin targeting of tau protein occurs at NFTs in the early and intermediate stages of the maturation.
机译:在神经原纤维缠结(NFT)的形成和成熟过程中,tau蛋白的病理过程包括异常磷酸化,构象变化和C末端天冬氨酸421(凋亡产物)和谷氨酸391残基的截短。异常的磷酸化和错误折叠可能充当针对泛素的靶向和蛋白体加工的识别信号。因此,我们试图确定以泛素为靶点的tau是否与特定的tau修饰有关,该修饰预示了阿尔茨海默氏病病例海马中NFT成熟的特定阶段。使用多种tau抗体,我们发现NFT的总负荷的30%与泛素相关。如先前报道,泛素的免疫反应性与某些NFTs中磷酸化tau的标记物有关。然而,在遍在蛋白和最早已知的天冬氨酸421截短事件之间也发现了很强的联系。这些发现表明NFT中的tau蛋白可能同时经历了凋亡和蛋白体加工。相比之下,遍在蛋白的免疫反应性与谷氨酸391处tau的截断关系不大,这表明这种蛋白水解事件可能与蛋白体活性无关。因此,看起来tau蛋白的泛素靶向发生在成熟的早期和中期的NFT处。

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