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Soluble Tau has devastating effects on the structural plasticity of hippocampal granule neurons

机译:可溶性Tau对海马颗粒神经元的结构可塑性具有破坏性作用

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Tau is a neuronal microtubule-associated protein with countless physiological functions. Although the detrimental effects of insoluble aggregated Tau have been widely studied, recent evidence supports the notion that soluble Tau (composed mostly of monomers and dimers) is also toxic for neurons. Here we evaluated the long-term impact of a single stereotaxic injection of human soluble Tau on hippocampal granule neurons in mice. At the ultrastructural level, soluble Tau reduced the number of afferent synapses and caused a dramatic depletion of synaptic vesicles both in afferent and efferent synapses. Furthermore, the use of an RFP-expressing retrovirus revealed that soluble Tau altered the morphology of newborn granule neurons and reduced their afferent (dendritic spines) and efferent (mossy fiber terminals) connectivity. Finally, soluble Tau caused specific impairment of behavioral pattern separation capacity. Our results thus demonstrate for the first time that soluble Tau causes long-term detrimental effects on the morphology and connectivity of newborn granule neurons and that these effects correlate with impaired behavioral pattern separation skills. These data might be relevant for the field of neurodegenerative disorders, since they contribute to reinforcing the pathological roles played by distinct Tau species in vivo .
机译:Tau是一种具有无数生理功能的神经元微管相关蛋白。尽管已经广泛研究了不溶性聚集Tau的有害作用,但最近的证据支持以下观点:可溶性Tau(主要由单体和二聚体组成)对神经元也有毒。在这里,我们评估了人类可溶的Tau的立体定位注射对小鼠海马颗粒神经元的长期影响。在超微结构水平,可溶性Tau减少了传入突触的数量,并导致传入和传出突触中突触小泡的急剧消耗。此外,使用表达RFP的逆转录病毒显示可溶性Tau改变了新生儿颗粒神经元的形态,并降低了它们的传入(树突棘)和传出(生苔纤维末端)的连接性。最后,可溶性Tau导致行为模式分离能力的特定损害。因此,我们的结果首次证明了可溶性Tau对新生颗粒神经元的形态和连通性产生了长期有害影响,并且这些影响与行为模式分离能力受损有关。这些数据可能与神经退行性疾病领域有关,因为它们有助于加强不同的Tau物种在体内发挥的病理作用。

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