Neuronal repair after spinal cord injury by in vivo astrocyte reprogramming mediated by the overexpression of NeuroD1 and Neurogenin-2

IF 4.3 2区 生物学 Q1 BIOLOGY
Zuliyaer Talifu, Chunjia Zhang, Xin Xu, Yunzhu Pan, Han Ke, Zehui Li, Wubo Liu, Huayong Du, Xiaoxin Wang, Feng Gao, Degang Yang, Yingli Jing, Yan Yu, Liangjie Du, Jianjun Li
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引用次数: 0

Abstract

As a common disabling disease, irreversible neuronal death due to spinal cord injury (SCI) is the root cause of functional impairment; however, the capacity for neuronal regeneration in the developing spinal cord tissue is limited. Therefore, there is an urgent need to investigate how defective neurons can be replenished and functionally integrated by neural regeneration; the reprogramming of intrinsic cells into functional neurons may represent an ideal solution. A mouse model of transection SCI was prepared by forceps clamping, and an adeno-associated virus (AAV) carrying the transcription factors NeuroD1 and Neurogenin-2(Ngn2) was injected in situ into the spinal cord to specifically overexpress these transcription factors in astrocytes close to the injury site. 5-bromo-2´-deoxyuridine (BrdU) was subsequently injected intraperitoneally to continuously track cell regeneration, neuroblasts and immature neurons marker expression, neuronal regeneration, and glial scar regeneration. In addition, immunoprotein blotting was used to measure the levels of transforming growth factor-β (TGF-β) pathway-related protein expression. We also evaluated motor function, sensory function, and the integrity of the blood-spinal cord barrier(BSCB). The in situ overexpression of NeuroD1 and Ngn2 in the spinal cord was achieved by specific AAV vectors. This intervention led to a significant increase in cell regeneration and the proportion of cells with neuroblasts and immature neurons cell properties at the injury site(p < 0.0001). Immunofluorescence staining identified astrocytes with neuroblasts and immature neurons cell properties at the site of injury while neuronal marker-specific staining revealed an increased number of mature astrocytes at the injury site. Behavioral assessments showed that the intervention did not improve The BMS (Basso mouse scale) score (p = 0.0726) and gait (p > 0.05), although the treated mice had more sensory sensitivity and greater voluntary motor ability in open field than the non-intervention mice. We observed significant repair of the BSCB at the center of the injury site (p < 0.0001) and a significant improvement in glial scar proliferation. Electrophysiological assessments revealed a significant improvement in spinal nerve conduction (p < 0.0001) while immunostaining revealed that the levels of TGF-β protein at the site of injury in the intervention group were lower than control group (p = 0.0034); in addition, P70 s6 and PP2A related to the TGF-β pathway showed ascending trend (p = 0.0036, p = 0.0152 respectively). The in situ overexpression of NeuroD1 and Ngn2 in the spinal cord after spinal cord injury can reprogram astrocytes into neurons and significantly enhance cell regeneration at the injury site. The reprogramming of astrocytes can lead to tissue repair, thus improving the reduced threshold and increasing voluntary movements. This strategy can also improve the integrity of the blood-spinal cord barrier and enhance nerve conduction function. However, the simple reprogramming of astrocytes cannot lead to significant improvements in the striding function of the lower limbs.
通过过表达 NeuroD1 和 Neurogenin-2 介导的体内星形胶质细胞重编程修复脊髓损伤后的神经元
作为一种常见的致残性疾病,脊髓损伤(SCI)导致的不可逆神经元死亡是功能障碍的根本原因;然而,发育中的脊髓组织的神经元再生能力有限。因此,迫切需要研究如何通过神经再生来补充有缺陷的神经元并实现功能整合;将固有细胞重编程为功能神经元可能是一个理想的解决方案。通过钳夹法制备了小鼠横断性脊髓损伤(SCI)模型,并将携带转录因子NeuroD1和Neurogenin-2(Ngn2)的腺相关病毒(AAV)原位注射到脊髓中,以特异性地在损伤部位附近的星形胶质细胞中过表达这些转录因子。随后腹腔注射 5-溴-2´-脱氧尿苷(BrdU)以持续跟踪细胞再生、神经母细胞和未成熟神经元标记表达、神经元再生和胶质疤痕再生。此外,我们还使用免疫蛋白印迹法测量了转化生长因子-β(TGF-β)通路相关蛋白的表达水平。我们还评估了运动功能、感觉功能和血脊髓屏障(BSCB)的完整性。脊髓中NeuroD1和Ngn2的原位过表达是通过特异性AAV载体实现的。与未干预小鼠相比,干预小鼠的感觉灵敏度更高,野外自主运动能力更强。我们观察到损伤部位中心的 BSCB 有明显修复(p < 0.0001),胶质疤痕增生也有明显改善。免疫染色显示,干预组损伤部位的 TGF-β 蛋白水平低于对照组(p = 0.0034);此外,与 TGF-β 通路相关的 P70 s6 和 PP2A 呈上升趋势(分别为 p = 0.0036 和 p = 0.0152)。在脊髓损伤后的脊髓中原位过表达 NeuroD1 和 Ngn2 可将星形胶质细胞重编程为神经元,并显著促进损伤部位的细胞再生。星形胶质细胞的重编程可导致组织修复,从而改善降低的阈值并增加自主运动。这一策略还能改善血脊髓屏障的完整性,增强神经传导功能。然而,单纯的星形胶质细胞重编程并不能显著改善下肢的跨步功能。
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来源期刊
Biological Research
Biological Research 生物-生物学
CiteScore
10.10
自引率
0.00%
发文量
33
审稿时长
>12 weeks
期刊介绍: Biological Research is an open access, peer-reviewed journal that encompasses diverse fields of experimental biology, such as biochemistry, bioinformatics, biotechnology, cell biology, cancer, chemical biology, developmental biology, evolutionary biology, genetics, genomics, immunology, marine biology, microbiology, molecular biology, neuroscience, plant biology, physiology, stem cell research, structural biology and systems biology.
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