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Approaches to therapy against prion diseases focused on the individual defence system

机译:针对病毒疾病的治疗方法侧重于个人防御系统

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Prion diseases are neurodegenerative disorders for which no effective treatment is available to date. Misfolded protein as aetiological agent is currently the most accepted theory. This review is focused on the hypothesis that the main basis of the progress of these disorders might fall on the individual defence system. Host protective response could convert into the early cellular event that triggers further brain tissue destruction. Specifically, neuroglial cells as main immunological cells located in brain might be influence on the pathogenic process of neurodegeneration by interaction with neurons. As consequence, neuroglia would be established as a turning point in therapeutic strategy of prion diseases. This alternative seems particularly desirable due to that they would result more effective than curative treatments trying to act on the irreversible neurodegenerating process. Moreover, all advances attained in the frame of this therapeutical approach result especially relevant for other neurodegenerative diseases such as Alzheimer’s, Parkinson’s or Huntington’s diseases, Frontotemporal dementia or Amyotrophic Lateral Sclerosis which are currently considered prion-like disorders since aberrant proteins spread throughout the brain during disease progression in all of them, and thus they may share molecular basis and mechanisms of propagation.
机译:on病毒疾病是神经退行性疾病,迄今为止尚无有效的治疗方法。错折叠的蛋白质作为病因是目前最被接受的理论。这篇综述集中在以下假设上:这些疾病进展的主要基础可能取决于个人防御系统。宿主的保护性反应可能会转变成早期的细胞事件,从而引发进一步的脑组织破坏。特别地,神经胶质细胞作为位于大脑中的主要免疫细胞,可能通过与神经元的相互作用而影响神经变性的致病过程。结果,神经胶质细胞将被确立为病毒疾病治疗策略的转折点。这种选择似乎是特别可取的,因为它们比试图对不可逆神经退化过程起作用的治疗方法更有效。此外,在这种治疗方法范围内取得的所有进展特别与其他神经退行性疾病(例如阿尔茨海默氏病,帕金森氏病或亨廷顿氏病,额颞痴呆或肌萎缩性侧索硬化症有关),这些疾病目前被视为病毒样疾病,因为异常蛋白在整个过程中遍布大脑它们都在疾病中发展,因此它们可能共享分子基础和传播机制。

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