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Daily bone marrow cell transplantations for the management of fast neurodegenerative processes

机译:每日骨髓细胞移植用于管理快速神经退行过程

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Abstract Cell therapy has been proven to be a promising treatment for fighting neurodegenerative diseases. As neuronal replacement presents undeniable complications, the neuroprotection of live neurons arises as the most suitable therapeutic approach. Accordingly, the earlier the diagnosis and treatment, the better the prognosis. However, these diseases are commonly diagnosed when symptoms have already progressed towards an irreversible degenerative stage. This problem is especially dramatic when neurodegeneration is aggressive and rapidly progresses. One of the most interesting approaches for neuroprotection is the fusion between healthy bone marrow‐derived cells and neurons, as the former can provide the latter with regular/protective genes without harming brain parenchyma. So far, this phenomenon has only been identified in Purkinje cells, whose death is the cause of different diseases like cerebellar ataxias. Here we have employed a model of aggressive cerebellar neurodegeneration, the Purkinje Cell Degeneration mouse, to optimize a cell therapy based on bone marrow‐derived cell and cell fusion. Our findings show that the substitution of bone marrow in diseased animals by healthy bone marrow, even prior to the onset of neurodegeneration, is not fast enough to stop neuronal loss in time. Conversely, avoiding bone marrow replacement and ensuring a regular supply of healthy cells through continuous, daily transplants, the neurodegenerative milieu of PCD is enough to attract those transplanted elements. Furthermore, in the most affected cerebellar regions, more than a half of surviving neurons undergo a process of cell fusion. Therefore, this method deserves consideration as a means to impede neuronal cell death.
机译:摘要被证明是对抗神经退行性疾病的有希望的疗法。随着神经元替代呈现不可否认的并发症,活神经元的神经保护作用是最合适的治疗方法。因此,较早的诊断和治疗,预后越好。然而,当症状已经朝着不可逆转的退行性阶段进行了症状时,这些疾病通常被诊断出来。当神经变性侵略性并且迅速进展时,这个问题特别戏剧性。神经保护的最有趣方法之一是健康骨髓衍生细胞和神经元之间的融合,因为前者可以提供常规/保护基因的后者而不伤害脑实质。到目前为止,这种现象仅在Purkinje细胞中鉴定,其死亡是不同疾病的原因,如小脑共济失调。在这里,我们使用了一种侵袭性小脑神经变性模型,紫癜细胞变性小鼠,以优化基于骨髓衍生细胞和细胞融合的细胞疗法。我们的研究结果表明,甚至在神经变性的发作之前,甚至在神经变性发作之前,甚至在患有神经变性的患者中替代骨髓,不足以阻止神经元损失。相反,避免骨髓替代并确保通过连续,每日移植的常规供应健康细胞,PCD的神经变性Milieu足以吸引那些移植的元素。此外,在最受影响的小脑区域中,超过一半的存活神经元经历了细胞融合的过程。因此,该方法应该考虑妨碍神经元细胞死亡的手段。

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