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tau 基因敲除可改善实验性创伤性脑损伤后小鼠的长期而非短期功能预后。

The genetic ablation of tau improves long-term, but not short-term, functional outcomes after experimental traumatic brain injury in mice.

机构信息

Department of Medicine, The Royal Melbourne Hospital, The University of Melbourne, Parkville, Australia.

Department of Neuroscience, Central Clinical School, Monash University, Melbourne, Australia.

出版信息

Brain Inj. 2020;34(1):131-139. doi: 10.1080/02699052.2019.1667539. Epub 2019 Sep 16.

Abstract

PRIMARY OBJECTIVE

This study characterized the acute and chronic effects of tau reduction in traumatic brain injury (TBI).

RESEARCH DESIGN

A fluid percussion injury (FPI) or a sham-injury was administered to wild type (WT) or tau knockout (Tau-/-) mice. Mice were assigned to a one-week or twelve-week recovery period before behavioral testing and analysis of brain tissue.

METHODS AND PROCEDURES

Mice were tested on the elevated-plus maze, the Y-maze, and rotarod. The twelve-week recovery mice underwent in vivo MRI. Phosphorylated tau in brain tissue was analyzed post-mortem using western blots.

MAIN OUTCOMES AND RESULTS

FPI mice, regardless of genotype, had abnormalities on the elevated-plus maze (a task to assess anxiety-like behavior) at one-week post-injury. However, after twelve-weeks recovery, the Tau-/- mice that were given an FPI were less anxious and had improved motor function compared to their WT counterparts. MRI analysis found that while all FPI mice had brain damage, the Tau-/- mice had larger hippocampal volumes. The WT+FPI mice also had increased phosphorylated tau compared to WT+sham mice at both the one-week and twelve-week recovery times.

CONCLUSION

These findings suggest that tau may play an important role in some of the consequences of TBI, particularly the long-term functional deficits.

摘要

主要目标

本研究旨在描述 Tau 减少对创伤性脑损伤 (TBI) 的急性和慢性影响。

研究设计

对野生型 (WT) 或 Tau 敲除 (Tau-/-) 小鼠进行液压冲击伤 (FPI) 或假损伤。在行为测试和脑组织分析之前,将小鼠分配到一周或十二周的恢复期。

方法和程序

在高架十字迷宫、Y 迷宫和转棒上对小鼠进行测试。十二周恢复期的小鼠接受体内 MRI 检查。使用 Western blot 分析死后脑组织中的磷酸化 Tau。

主要结果和结论

无论基因型如何,FPI 小鼠在损伤后一周的高架十字迷宫(评估焦虑样行为的任务)上均出现异常。然而,在十二周的恢复期后,接受 FPI 的 Tau-/- 小鼠的焦虑程度低于其 WT 对应物,运动功能也得到改善。MRI 分析发现,虽然所有 FPI 小鼠都有脑损伤,但 Tau-/- 小鼠的海马体积更大。WT+FPI 小鼠在一周和十二周恢复期的磷酸化 Tau 水平也高于 WT+sham 小鼠。

这些发现表明,Tau 可能在 TBI 的一些后果中发挥重要作用,特别是长期的功能缺陷。

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