James P Quinn, Kate Fisher, Nicola Corbett, Stacey Warwood, David Knight, Katherine A B Kellett, Nigel M Hooper
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引用次数: 0
Abstract
Tauopathies, including Alzheimer's disease, corticobasal degeneration and progressive supranuclear palsy, are characterised by the aggregation of tau into insoluble neurofibrillary tangles in the brain. Tau is subject to a range of post-translational modifications, including proteolysis, that can promote its aggregation. Neuroinflammation is a hallmark of tauopathies and evidence is growing for a role of CD8+ T cells in disease pathogenesis. CD8+ T cells release granzyme proteases but what role these proteases play in neuronal dysfunction is currently lacking. Here, we identified that granzyme A (GzmA) is present in brain tissue and proteolytically cleaves tau. Mass spectrometric analysis of tau fragments produced on digestion of tau with GzmA identified three cleavage sites at R194-S195, R209-S210 and K240-S241. Mutation of the critical Arg or Lys residues at the cleavage sites in tau or chemical inhibition of GzmA blocked the proteolysis of tau by GzmA. Development of a semi-targeted mass spectrometry approach identified peptides in tauopathy brain tissue corresponding to proteolysis by GzmA at R209-S210 and K240-S241 in tau. When expressed in cells the GzmA-cleaved C-terminal fragments of tau were highly phosphorylated and aggregated upon incubation of the cells with tauopathy brain seed. The C-terminal fragment tau195-441 was able to transfer between cells and promote aggregation of tau in acceptor cells, indicating the propensity for such tau fragments to propagate between cells. Collectively, these results raise the possibility that GzmA, released from infiltrating cytotoxic CD8+ T cells, proteolytically cleaves tau into fragments that may contribute to its pathological properties in tauopathies.
Tau 病(包括阿尔茨海默病、皮质基底变性和进行性核上性麻痹)的特征是 Tau 在大脑中聚集成不溶性的神经纤维缠结。Tau 会发生一系列翻译后修饰,包括蛋白水解,从而促进其聚集。神经炎症是 Tau 病的特征之一,越来越多的证据表明 CD8+ T 细胞在疾病发病机制中发挥作用。CD8+ T 细胞会释放颗粒酶蛋白酶,但这些蛋白酶在神经元功能障碍中扮演何种角色目前尚不清楚。在这里,我们发现颗粒酶 A(GzmA)存在于脑组织中,并能蛋白水解 tau。用GzmA消化tau后产生的tau片段的质谱分析确定了R194-S195、R209-S210和K240-S241三个裂解位点。突变tau裂解位点上的关键Arg或Lys残基或对GzmA进行化学抑制都会阻止GzmA对tau的蛋白水解。半靶向质谱方法的开发确定了tau病脑组织中与GzmA在tau的R209-S210和K240-S241处蛋白水解作用相对应的肽段。在细胞中表达时,GzmA裂解的tau C端片段会高度磷酸化,并在细胞与tauopathy脑种子培养后聚集。C末端片段tau195-441能够在细胞间转移,并促进接受细胞中tau的聚集,这表明这种tau片段有在细胞间传播的倾向。总之,这些结果提出了一种可能性,即浸润的细胞毒性CD8+ T细胞释放的GzmA能将tau蛋白水解为片段,而这些片段可能会导致tau病的病理特性。
期刊介绍:
Exploring the molecular mechanisms that underpin key biological processes, the Biochemical Journal is a leading bioscience journal publishing high-impact scientific research papers and reviews on the latest advances and new mechanistic concepts in the fields of biochemistry, cellular biosciences and molecular biology.
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