Department of Biochemistry & Nutrition, CSIR-Central Food Technological Research Institute (CFTRI), Mysore, 570020, India.
Cell Mol Neurobiol. 2013 Oct;33(7):929-42. doi: 10.1007/s10571-013-9959-y. Epub 2013 Jul 19.
Oxidative stress is one of the mechanisms implicated to play a significant role in the pathophysiology of Parkinson's disease. Previously, we showed that an aqueous extract of Selaginella delicatula (SDAE) offered robust neuroprotection against rotenone (ROT) in a Drosophila model. In furtherance in the present study, we validated the neuroprotective efficacy of SDAE in a chronic ROT exposure model in mice. Initially, we assessed the propensity of SDAE to modulate the levels of endogenous markers in striatal region of mice. Subsequently, the neuroprotective efficacy of SDAE (100 mg/kg bw, 21 d) to mitigate ROT-induced striatal motor deficits, oxidative stress, and neurotoxicity was examined employing a co-exposure paradigm. We found significant attenuation of ROT-induced motor deficits (stride length and landing foot spread distance) among mice given SDAE supplements. Biochemical analysis revealed that ROT-induced elevation in the levels of oxidative markers in cytosol/mitochondria of striatum were normalized with SDAE supplements. In addition, SDAE also restored the ROT-induced elevation in the levels of oxidized and nitrated proteins. Further, SDAE also restored the activities of acetylcholinesterase and butyrylcholinesterase indicating its effect on cholinergic function. While ROT exposure caused significant perturbations in the activity levels of mitochondrial electron transport chain enzymes (complex I/II), membrane potential and activity of ATPases, these functions were restored to normalcy among mice receiving SDAE suggesting its effects on mitochondrial function. Since these data corroborate our previous findings in Drosophila system, we propose that the neuroprotective property of SDAE may be largely attributed to the antioxidant properties and its ability to attenuate mitochondrial dysfunction. However, studies employing dopaminergic cell models would enable us to identify specific molecular mechanism, by which SDAE exerts neuroprotective action.
氧化应激是帕金森病病理生理学中起重要作用的机制之一。此前,我们表明,翠云草(SDAE)的水提物在果蝇模型中对鱼藤酮(ROT)表现出强大的神经保护作用。在本研究中,我们进一步验证了 SDAE 在慢性 ROT 暴露模型中小鼠中的神经保护作用。最初,我们评估了 SDAE 调节小鼠纹状体区域内源性标志物水平的倾向。随后,采用共暴露范式研究了 SDAE(100mg/kg bw,21d)减轻 ROT 诱导的纹状体运动缺陷、氧化应激和神经毒性的神经保护作用。我们发现,给予 SDAE 补充剂的小鼠,其 ROT 诱导的运动缺陷(步幅长度和着陆脚距)明显减弱。生化分析表明,SDAE 补充剂可使 ROT 诱导的纹状体细胞质/线粒体中氧化标记物水平升高得到正常化。此外,SDAE 还恢复了 ROT 诱导的氧化和硝化蛋白水平升高。此外,SDAE 还恢复了乙酰胆碱酯酶和丁酰胆碱酯酶的活性,表明其对胆碱能功能的影响。虽然 ROT 暴露导致线粒体电子传递链酶(复合物 I/II)、膜电位和 ATP 酶活性的水平发生显著变化,但接受 SDAE 治疗的小鼠这些功能恢复正常,表明 SDAE 对线粒体功能的影响。由于这些数据与我们在果蝇系统中的先前发现相符,我们提出 SDAE 的神经保护特性可能主要归因于其抗氧化特性及其减轻线粒体功能障碍的能力。然而,采用多巴胺能细胞模型的研究将使我们能够确定 SDAE 发挥神经保护作用的特定分子机制。
