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Amelioration of acute and relapsing stages of the experimental allergic encephalomyelitis by cobra toxins.

机译:通过眼镜蛇毒素改善实验性变应性脑脊髓炎的急性和复发期。

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摘要

Neurological deficits in multiple sclerosis (MS) and in experimental allergic encephalomyelitis (EAE) show demyelination of the nerve fibers, which are responsible for transmission of signals. The myelin appears to be attacked by the cells of the immune system. A viral etiology has been implicated in patients with MS. Oxidized toxins (MN) have been shown over the past 50 years to act as antiviral agents that are capable of inhibiting viral replication, and have shown promise in alleviating symptoms in EAE models of MS. The safety of these compounds has been a factor in their limited use. Development of a modified cobra toxin (MCTX) may prove more beneficial in inhibiting symptoms of EAE. In this study a modified cobra toxin (MCTX) was compared with the older oxidized toxin (MN) in an established EAE animal model. The results show that MCTX is capable of inhibiting the development as well as the relapsing phase of EAE in Lewis rats more efficiently than MN. It is possible that a safe cobra toxin can be developed with therapeutic efficacy for treatment of MS or vaccine development.
机译:多发性硬化症(MS)和实验性变应性脑脊髓炎(EAE)中的神经功能缺损显示神经纤维脱髓鞘,这负责信号的传递。髓磷脂似乎受到免疫系统细胞的攻击。 MS患者中涉及病毒病因。在过去的50年中,氧化毒素(MN)已被证明可以作为抗病毒剂,能够抑制病毒复制,并有望缓解MS的EAE模型中的症状。这些化合物的安全性是其有限使用的一个因素。修饰眼镜蛇毒素(MCTX)的开发可能在抑制EAE症状方面更有益。在这项研究中,在建立的EAE动物模型中将修饰的眼镜蛇毒素(MCTX)与较旧的氧化毒素(MN)进行了比较。结果表明,MCTX能够比MN更有效地抑制Lewis大鼠EAE的发育和复发期。有可能开发出具有治疗MS或疫苗开发疗效的安全眼镜蛇毒素。

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