Rehabilitation training enhanced the therapeutic effect of calycosin on neurological function recovery of rats following spinal cord injury

IF 2.7 4区 医学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Mingdong Li , Yanqiang Huan , Tianqi Jiang , Yongxiong He , Zengxin Gao
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引用次数: 0

Abstract

Background

Calycosin (CA), a flavonoids component, has demonstrated potential neuroprotection effects by inhibiting oxidative stress in spinal cord injury (SCI) models. This study aims to investigate the impact of combined rehabilitation training (RT) and calycosin therapy on neurological function following SCI, primarily by assessing changes in motor function recovery, neuronal survival, neuronal oxidative stress levels, and neural proliferation, in order to provide novel insights for the treatment of SCI.

Materials and Methods

The SCI model was constructed by compressing the spinal cord using vascular clamps. Calycosin was injected intraperitoneally into the SCI model rats, and a group of 5 rats underwent RT. The motor function of rats after SCI was evaluated using the Basso Beattle Bresnaha (BBB) score and the inclined plate test. Histopathological changes were evaluated by NeuN immunohistochemistry, HE and Nissl staining. Apoptosis was detected by TUNEL staining. The antioxidant effect of combined treatment was assessed by measuring changes in oxidative stress markers after SCI. Western blot analysis was conducted to examine changes in Hsp90-Akt/ASK1-p38 pathway-related proteins. Finally, cell proliferation was detected by BrdU and Ki67 assays.

Results

RT significantly improved the BBB score and angle of incline promoted by calycosin, resulting in enhanced motor function recovery in rats with SCI. Combining rehabilitation training with calycosin has a positive effect on morphological recovery. Similarly, combined RT enhanced the Nissl and NeuN staining signals of spinal cord neurons increased by calycosin, thereby increasing the number of neurons. TUNEL staining results indicated that calycosin treatment reduced the apoptosis signal in SCI, and the addition of RT further reduced the apoptosis. Moreover, RT combined with calycosin reduced oxidative stress by increasing SOD and GSH levels, while decreasing MDA, NO, ROS, and LDH expressions compared to the calycosin alone. RT slightly enhanced the effect of calycosin in activating Hsp90 and Akt and inhibiting the activation of ASK1 and p38, leading to enhanced inhibition of oxidative stress by calycosin. Additionally, the proliferation indexes (Ki67 and BrdU) assays showed that calycosin treatment alone increased both, whereas the combination treatment further promoted cell proliferation.

Conclusion

Our research findings demonstrate that rehabilitation training enhances the ability of calycosin to reduce oxidative stress, resulting in a decrease in neuronal apoptosis and an increase in proliferation, ultimately promoting neuronal survival.

康复训练增强了钙苷对脊髓损伤后大鼠神经功能恢复的治疗效果。
背景:萼萼素是一种黄酮类成分,在脊髓损伤(SCI)模型中通过抑制氧化应激而显示出潜在的神经保护作用。本研究旨在通过评估运动功能恢复、神经元存活、神经元氧化应激水平和神经增殖等方面的变化,研究康复训练(RT)和萼苷联合疗法对脊髓损伤后神经功能的影响,从而为脊髓损伤的治疗提供新的见解:使用血管钳夹压迫脊髓,构建 SCI 模型。材料和方法:利用血管钳压迫脊髓,构建 SCI 模型,向 SCI 模型大鼠腹腔注射钙磷脂,每 5 只大鼠为一组进行 RT 治疗。使用巴索-贝托-布雷斯纳哈(BBB)评分和斜板试验评估大鼠脊髓损伤后的运动功能。组织病理学变化通过NeuN免疫组化、HE和Nissl染色进行评估。通过 TUNEL 染色检测细胞凋亡。通过测量 SCI 后氧化应激标记物的变化来评估联合治疗的抗氧化效果。进行了 Western 印迹分析,以检测 Hsp90-Akt/ASK1-p38 通路相关蛋白的变化。最后,通过 BrdU 和 Ki67 检测细胞增殖:结果:RT明显改善了BBB评分和钙黄素促进的倾斜角度,从而增强了SCI大鼠的运动功能恢复。康复训练与钙磷脂相结合对形态学恢复有积极作用。同样,联合 RT 可增强钙磷脂增加的脊髓神经元的 Nissl 和 NeuN 染色信号,从而增加神经元的数量。TUNEL 染色结果表明,钙调磷酸治疗可减少 SCI 中的细胞凋亡信号,而 RT 的加入可进一步减少细胞凋亡。此外,与单独使用钙泊三醇相比,RT与钙泊三醇联合使用可提高SOD和GSH水平,降低MDA、NO、ROS和LDH的表达,从而减少氧化应激。RT 稍微增强了钙磷脂激活 Hsp90 和 Akt 的作用,抑制了 ASK1 和 p38 的激活,从而增强了钙磷脂对氧化应激的抑制作用。此外,增殖指标(Ki67和BrdU)检测显示,单独使用钙苷处理可增加细胞增殖,而联合使用可进一步促进细胞增殖:我们的研究结果表明,康复训练能增强钙调素降低氧化应激的能力,从而减少神经元凋亡,增加细胞增殖,最终促进神经元存活。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of chemical neuroanatomy
Journal of chemical neuroanatomy 医学-神经科学
CiteScore
4.50
自引率
3.60%
发文量
87
审稿时长
62 days
期刊介绍: The Journal of Chemical Neuroanatomy publishes scientific reports relating the functional and biochemical aspects of the nervous system with its microanatomical organization. The scope of the journal concentrates on reports which combine microanatomical, biochemical, pharmacological and behavioural approaches. Papers should offer original data correlating the morphology of the nervous system (the brain and spinal cord in particular) with its biochemistry. The Journal of Chemical Neuroanatomy is particularly interested in publishing important studies performed with up-to-date methodology utilizing sensitive chemical microassays, hybridoma technology, immunocytochemistry, in situ hybridization and receptor radioautography, to name a few examples. The Journal of Chemical Neuroanatomy is the natural vehicle for integrated studies utilizing these approaches. The articles will be selected by the editorial board and invited reviewers on the basis of their excellence and potential contribution to this field of neurosciences. Both in vivo and in vitro integrated studies in chemical neuroanatomy are appropriate subjects of interest to the journal. These studies should relate only to vertebrate species with particular emphasis on the mammalian and primate nervous systems.
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