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可溶性Nogo-A,一种轴突再生抑制剂,作为多发性硬化症的生物标志物。

Soluble Nogo-A, an inhibitor of axonal regeneration, as a biomarker for multiple sclerosis.

作者信息

Jurewicz Anna, Matysiak Mariola, Raine Cedric S, Selmaj Krzysztof

机构信息

Department of Neurology, Medical University of Lodz, 22, Kopcińskiego Street, 90-153 Lodz, Poland.

出版信息

Neurology. 2007 Jan 23;68(4):283-7. doi: 10.1212/01.wnl.0000252357.30287.1d.

Abstract

BACKGROUND

CNS axons display a poor regenerative response to injury. In multiple sclerosis (MS), failure of damaged axons to regenerate may be a major factor underlying non-reversible neurologic dysfunction. Nogo is a development-related molecule inhibiting axonal regeneration and is a major component of CNS myelin.

METHODS

CSF from 114 patients with remitting relapsing MS (RR-MS) and secondary progressive MS (SP-MS) and 153 controls, as well as CNS tissue from 3 patients with MS and 2 controls, were used for this study.

RESULTS

We found soluble 20 kDa Nogo-A product in 96% (110/114) of CSF samples from patients with MS compared with 0/18 from meningo-encephalomyelitis, 0/125 from control subjects with other neurologic diseases, and 0/10 from CNS autoimmune diseases. Nogo-A products were present both in RR-MS and SP-MS, as well as in early cases of the disease, but not in neuromyelitis optica. The same Nogo A product was detected in CNS tissue from all patients with MS but not in control CNS tissue.

CONCLUSION

Soluble Nogo-A may be specific for the CSF of patients with multiple sclerosis and its presence may predict failure of axonal regeneration within the CNS.

摘要

背景

中枢神经系统(CNS)轴突损伤后再生反应较差。在多发性硬化症(MS)中,受损轴突无法再生可能是导致不可逆神经功能障碍的主要因素。Nogo是一种与发育相关的分子,可抑制轴突再生,是中枢神经系统髓鞘的主要成分。

方法

本研究使用了114例复发缓解型MS(RR-MS)和继发进展型MS(SP-MS)患者以及153例对照者的脑脊液,以及3例MS患者和2例对照者的中枢神经系统组织。

结果

我们在96%(110/114)的MS患者脑脊液样本中发现了可溶性20 kDa Nogo-A产物,而在脑膜脑脊髓炎患者的脑脊液样本中该比例为0/18,其他神经系统疾病对照者的脑脊液样本中该比例为0/125,中枢神经系统自身免疫性疾病患者的脑脊液样本中该比例为0/10。Nogo-A产物在RR-MS和SP-MS患者中均有存在,在疾病早期病例中也有发现,但在视神经脊髓炎患者中未发现。在所有MS患者的中枢神经系统组织中均检测到相同的Nogo A产物,而对照中枢神经系统组织中未检测到。

结论

可溶性Nogo-A可能是多发性硬化症患者脑脊液所特有的,其存在可能预示着中枢神经系统内轴突再生失败。

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