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循环神经生长因子抗体改变炎症性疾病动物模型大脑中NG2和CD56阳性细胞的分布。

Circulating NGF antibody alters the distribution of NG2 and CD56 positive cells in the brain of an animal model of inflammatory disorder.

作者信息

Triaca V, Tirassa P

机构信息

Institute of Neurobiology CNR, Viale Marx 15, 00137, Rome, Italy.

出版信息

Arch Ital Biol. 2003 Mar;141(2-3):127-39.

Abstract

Using an animal model of endogenous Nerve Growth Factor (NGF) deprivation, we have investigated the effect of this molecule on the distribution of NG2 and CD56-positive cells in the brain of normal and of Experimental Allergic Encephalomyelitis (EAE) rats. We found that the number of these cells is significantly altered in the SubVentricular Zone (SVZ) and in other brain regions. These findings indicate that NGF might be implicated in the regulation of the antigen expressed by oligodendrocyte progenitors (NG2) and of the neural cell adhesion molecule (CD56/NCAM). Both antigens are associated with mechanisms of brain repair thus providing additional evidence for a major role of NGF in the brain response to pathological conditions such as EAE. Acknowledgements.--We thank Prof. R. Levi-Montalcini for her stimulating discussions. We also thank Dr. L. Aloe for critical reading of the manuscript. This study was supported by Proj. Strategico CNR, by AISM and by Fondazione CARISBO, Bologna. Dr. V. Triaca is a recipient of a fellowship from the AISM.

摘要

利用内源性神经生长因子(NGF)剥夺的动物模型,我们研究了该分子对正常大鼠和实验性自身免疫性脑脊髓炎(EAE)大鼠大脑中NG2和CD56阳性细胞分布的影响。我们发现,这些细胞的数量在脑室下区(SVZ)和其他脑区有显著变化。这些发现表明,NGF可能参与少突胶质前体细胞(NG2)表达的抗原以及神经细胞黏附分子(CD56/NCAM)的调节。这两种抗原都与脑修复机制相关,从而为NGF在大脑对诸如EAE等病理状况的反应中起主要作用提供了额外证据。致谢。——我们感谢R. 莱维-蒙塔尔奇尼教授富有启发性的讨论。我们也感谢L. 阿洛博士对手稿的严格审阅。本研究得到了意大利国家研究委员会战略项目、意大利多发性硬化症协会(AISM)和博洛尼亚卡里索基金会的支持。V. 特里阿卡博士获得了意大利多发性硬化症协会的奖学金。

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