Isoform-specific upregulation of FynT kinase expression is associated with tauopathy and glial activation in Alzheimer's disease and Lewy body dementias

Michelle G. K. Tan, Mitchell K. P. Lai, Paul T. Francis, C. Ballard, Chingli Lee, Frances T. W. Lim, Jasinda H. Lee, Clara Y. B. Low
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Abstract

Cumulative data suggest the involvement of Fyn tyrosine kinase in Alzheimer's disease (AD). Previously, our group has shown increased immunoreactivities of the FynT isoform in AD neocortex (with no change in the alternatively spliced FynB isoform) which associated with neurofibrillary degeneration and reac-tive astrogliosis. Since both the aforementioned neuropathological features are also variably found in Lewy Body dementias (LBD), we investigated potential perturbations of Fyn expression in the post-mortem neocortex of patients with AD, as well as those diagnosed as having one of the two main subgroups of LBD: Parkinson's disease dementia (PDD) and dementia with Lewy bodies (DLB). We found selective upregulation of FynT expression in AD, PDD, and DLB which also correlated with cognitive impairment. Furthermore, increased FynT expression correlated with hallmark neuropathological lesions, soluble β-amyloid, and phosphorylated tau, as well as markers of microglia and as-trocyte activation. In line with the human post-mortem studies, cortical FynT expression in aged mice transgenic for human P301S tau was upregulated and further correlated with accumulation of aggregated phosphorylated tau as well as with microglial and astrocytic markers. Our findings provide further evi-dence for the involvement of FynT in neurodegenerative dementias, likely via effects on tauopathy and neuroinflammation.
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FynT激酶表达的异构体特异性上调与阿尔茨海默病和路易体痴呆的tau病变和神经胶质活化有关
累积数据表明Fyn酪氨酸激酶参与阿尔茨海默病(AD)。在此之前,我们的研究小组已经发现,与神经原纤维变性和反应性星形胶质增生相关的FynT亚型在阿尔茨海默病新皮层中的免疫反应性增加(FynB亚型的选择性剪接没有变化)。由于上述两种神经病理特征在路易体痴呆(LBD)中也有不同的发现,我们研究了AD患者死后新皮层中Fyn表达的潜在扰动,以及那些被诊断为LBD两个主要亚群之一的患者:帕金森病痴呆(PDD)和路易体痴呆(DLB)。我们发现FynT在AD、PDD和DLB中选择性表达上调,这也与认知障碍有关。此外,FynT表达的增加与标志性神经病理病变、可溶性β-淀粉样蛋白、磷酸化tau蛋白以及小胶质细胞和胶质细胞活化的标志物相关。与人类死后研究一致,转基因人类P301S tau的老年小鼠皮层FynT表达上调,并进一步与聚集磷酸化tau的积累以及小胶质和星形胶质细胞标志物相关。我们的研究结果为FynT参与神经退行性痴呆提供了进一步的证据,可能是通过对tau病和神经炎症的影响。
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