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通过腺相关病毒rg逆行转导在脊髓通路中删除PTEN可增强颈脊髓损伤后前肢运动恢复;性别差异和迟发性病理生理学

PTEN deletion in spinal pathways via retrograde transduction with AAV-rg enhances forelimb motor recovery after cervical spinal cord injury; sex differences and late-onset pathophysiologies.

作者信息

Metcalfe Mariajose, Steward Oswald

出版信息

bioRxiv. 2023 Jul 24:2023.03.20.533502. doi: 10.1101/2023.03.20.533502.

Abstract

Spinal cord injuries (SCI) cause permanent functional impairments due to interruption of motor and sensory pathways. Regeneration of axons does not occur due to lack of intrinsic growth capacity of adult neurons and extrinsic inhibitory factors, especially at the injury site. However, some regeneration can be achieved via deletion of the phosphatase and tensin homolog (PTEN) in cells of origin of spinal pathways. Here, we deployed an AAV variant that is retrogradely transported (AAV-rg) to deliver gene modifying cargos to the cells of origin of multiple pathways interrupted by SCI, testing whether this promoted recovery of motor function. PTEN ;Rosa mice and control Rosa mice received injections of different doses (number of genome copies, GCs) of AAV-rg/Cre into the cervical spinal cord at the time of a C5 dorsal hemisection injury. Forelimb grip strength was tested over time using a grip strength meter. PTEN ;Rosa mice with AAV-rg/Cre (PTEN-deleted) exhibited substantial improvements in forelimb gripping ability in comparison to controls. Of note, there were major sex differences in the extent of recovery, with male mice exhibiting greater recovery than females. However, at around 5-7 weeks post-injury/injection, many mice with SCI and AAV-rg-mediated PTEN deletion began to exhibit pathophysiologies involving excessive scratching of the ears and back of the neck and rigid forward extension of the hindlimbs. These pathophysiologies increased in incidence and severity over time. Our results reveal that although intra-spinal injections of AAV-rg/Cre in PTEN ;Rosa mice can enhance forelimb motor recovery after SCI, late-developing functional abnormalities occur with the experimental conditions used here. Mechanisms underlying late-developing pathophysiologies remain to be defined.

摘要

脊髓损伤(SCI)会因运动和感觉通路中断而导致永久性功能障碍。由于成年神经元缺乏内在生长能力以及存在外在抑制因子,尤其是在损伤部位,轴突无法再生。然而,通过缺失脊髓通路起源细胞中的磷酸酶和张力蛋白同源物(PTEN),可以实现一定程度的再生。在此,我们采用了一种可逆行运输的腺相关病毒变体(AAV-rg),将基因编辑载体递送至因SCI而中断的多条通路的起源细胞,以测试这是否能促进运动功能的恢复。在进行C5背侧半横断损伤时,PTENfl/fl;Rosa26tdTomato/+小鼠和对照Rosa26tdTomato/+小鼠接受了不同剂量(基因组拷贝数,GCs)的AAV-rg/Cre注射到颈脊髓。使用握力计随时间测试前肢握力。与对照组相比,接受AAV-rg/Cre(PTEN缺失)的PTENfl/fl;Rosa26tdTomato/+小鼠在前肢抓握能力方面有显著改善。值得注意的是,恢复程度存在主要的性别差异,雄性小鼠的恢复程度大于雌性小鼠。然而,在损伤/注射后约5 - 7周,许多患有SCI且经AAV-rg介导的PTEN缺失的小鼠开始出现病理生理学症状,包括过度抓挠耳朵和颈部后方以及后肢僵硬向前伸展。这些病理生理学症状的发生率和严重程度随时间增加。我们的结果表明,虽然在PTENfl/fl;Rosa26tdTomato/+小鼠中脊髓内注射AAV-rg/Cre可以增强SCI后的前肢运动恢复,但在此处使用的实验条件下会出现后期发展的功能异常。后期发展的病理生理学机制仍有待确定。

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