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在携带突变 tau 蛋白的小鼠神经元中,结构和功能的改变与 NFT 的出现无关。

Structural and functional changes in tau mutant mice neurons are not linked to the presence of NFTs.

机构信息

Department of Anatomy and Neurobiology, M949, Boston University School of Medicine, 85 E. Newton St., Boston, MA 02118, USA.

出版信息

Exp Neurol. 2010 Jun;223(2):385-93. doi: 10.1016/j.expneurol.2009.07.029. Epub 2009 Aug 7.

Abstract

In the rTg4510 mouse model, expression of the mutant human tau variant P301L leads to development of neurofibrillary tangles (NFTs), neuronal death, and memory impairment, reminiscent of the pathology observed in human tauopathies. In the present study, we examined the effects of mutant tau expression on the electrophysiology and morphology of individual neurons using whole-cell patch-clamp recordings and biocytin filling of pyramidal cells in cortical slices prepared from rTg4510 (TG) and wild-type (WT) littermate mice. Among the TG cells, 42% contained a clear Thioflavin-S positive inclusion in the soma and were categorized as NFT positive (NFT+), while 58% had no discernable inclusion and were categorized as NFT negative (NFT-). The resting membrane potential (V(r)) was significantly depolarized (+8 mV) in TG cells, and as a consequence, evoked repetitive action potential (AP) firing rates were also significantly increased. Further, single APs were significantly shorter in duration in TG cells and the depolarizing voltage deflection or "sag" evoked by hyperpolarization was significantly greater in amplitude. In addition to these functional electrophysiological changes, TG cells exhibited significant morphological alterations, including loss or significant atrophy of the apical tuft, reduced dendritic complexity and length, and reduced spine density. Importantly, NFT- and NFT+ TG cells were indistinguishable with regard to both morphological and electrophysiological properties. Our observations show that expression of mutated tau results in significant structural and functional changes in neurons, but that these changes occur independent of mature NFT formation.

摘要

在 rTg4510 小鼠模型中,突变人 tau 变体 P301L 的表达导致神经原纤维缠结(NFTs)、神经元死亡和记忆损伤的发展,类似于人类 tau 病中观察到的病理学。在本研究中,我们使用全细胞膜片钳记录和皮质切片中锥体神经元的生物胞素填充,检查突变 tau 表达对单个神经元的电生理学和形态的影响,这些切片是从 rTg4510(TG)和野生型(WT)同窝小鼠中制备的。在 TG 细胞中,42%的细胞在胞体中含有明显的 Thioflavin-S 阳性包涵体,并被归类为 NFT 阳性(NFT+),而 58%的细胞没有明显的包涵体,并被归类为 NFT 阴性(NFT-)。TG 细胞的静息膜电位(V(r))明显去极化(+8 mV),因此,诱发的重复动作电位(AP)发射率也显著增加。此外,TG 细胞中的单个 AP 持续时间明显缩短,超极化诱发的去极化电压偏移或“凹陷”幅度显著增大。除了这些功能电生理学变化外,TG 细胞还表现出明显的形态改变,包括顶树突丛的缺失或明显萎缩、树突复杂性和长度减少以及棘突密度降低。重要的是,NFT-和 NFT+TG 细胞在形态和电生理特性方面没有区别。我们的观察表明,突变 tau 的表达导致神经元发生显著的结构和功能变化,但这些变化发生在成熟 NFT 形成之前。

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