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Wallerian degeneration: a major component of early axonal pathology in multiple sclerosis.

机译:沃勒氏变性:多发性硬化症的早期轴突病理学的主要组成部分。

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摘要

Axonal loss is a major component of the pathology of multiple sclerosis (MS) and the morphological basis of permanent clinical disability. It occurs in demyelinating plaques but also in the so-called normal-appearing white matter (NAWM). However, the contribution of Wallerian degeneration to axonal pathology is not known. Here, we analyzed the extent of Wallerian degeneration and axonal pathology in periplaque white matter (PPWM) and lesions in early multiple sclerosis biopsy tissue from 63 MS patients. Wallerian degeneration was visualized using an antibody against the neuropeptide Y receptor Y1 (NPY-Y1R). The number of SMI-32-positive axons with non-phosphorylated neurofilaments was significantly higher in both PPWM and plaques compared to control white matter. APP-positive, acutely damaged axons were found in significantly higher numbers in plaques compared to PPWM. Strikingly, the number of NPY-Y1R-positive axons undergoing Wallerian degeneration was significantly higher in PPWM and plaques than in control WM. NPY-Y1R-positive axons in PPWM were strongly correlated to those in the lesions. Our results show that Wallerian degeneration is a major component of axonal pathology in the periplaque white matter in early MS. It may contribute to radiological changes observed in early MS and most likely plays a major role in the development of disability.
机译:轴突丢失是多发性硬化症(MS)病理的主要组成部分,也是永久性临床残疾的形态学基础。它出现在脱髓鞘斑块中,也出现在所谓的正常外观白质(NAWM)中。然而,沃勒变性对轴突病理学的贡献尚不清楚。在这里,我们分析了63名MS患者的斑块周围白质(PPWM)中Wallerian变性和轴突病理的程度以及早期多发性硬化活检组织中的病变。使用针对神经肽Y受体Y1(NPY-Y1R)的抗体观察Wallerian变性。与对照白质相比,PPWM和斑块中具有非磷酸化神经丝的SMI-32阳性轴突的数量明显更高。与PPWM相比,APP阳性,急性受损的轴突在斑块中的数量明显更高。令人惊讶的是,PPWM和斑块中经历Wallerian变性的NPY-Y1R阳性轴突的数量显着高于对照WM。 PPWM中的NPY-Y1R阳性轴突与病变中的轴突高度相关。我们的结果表明,沃勒氏变性是MS早期斑块周围白质轴突病理的主要成分。它可能有助于早期MS中观察到的放射学变化,并且很可能在残疾发展中起主要作用。

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