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飞摩尔作用的NAP与微管相互作用:星形胶质细胞保护的新方面。

The femtomolar-acting NAP interacts with microtubules: Novel aspects of astrocyte protection.

作者信息

Gozes Illana, Divinski Inna

机构信息

Department of Clinical Biochemistry, Sackler School of Medicine, Tel Aviv University, Tel Aviv 69978, Israel.

出版信息

J Alzheimers Dis. 2004 Dec;6(6 Suppl):S37-41. doi: 10.3233/jad-2004-6s605.

Abstract

Activity-dependent neuroprotective protein (ADNP), a gene product essential for brain formation, contains a short octapeptide sequence NAPVSIPQ (NAP) that protects neurons against a wide variety of insults. At the pico-molar concentration range, NAP provides neuroprotection by direct interaction with neurons. At the femtomolar concentration range, NAP requires the presence of glial cells to provide neuroprotection. To further understand the mechanism of neuroprotection afforded by NAP, specific binding proteins were searched for. Tubulin, the major subunit protein of microtubules, was identified as a NAP binding molecule. NAP structure allows membrane penetration, followed by tubulin binding and facilitation of microtubule assembly toward cellular protection in astrocytes. NAP (10(-15) M) promoted microtubule assembly in vitro and protected astrocytes against zinc intoxication which is associated with microtubule disruption. A two hour incubation period of astrocytes with femtomolar concentrations of NAP resulted in microtubule re-organization and transient increases in immunoreactive non-phosphorylated tau. Microtubules are the key component of the neuronal and glial cytoskeleton that regulates cell division, differentiation and protection, while tau pathology is a major contributor to Alzheimer's disease and other dementias. The findings described here may open up new horizons in research and development of neuroprotective compounds.

摘要

活性依赖的神经保护蛋白(ADNP)是大脑形成所必需的一种基因产物,它包含一个短的八肽序列NAPVSIPQ(NAP),该序列能保护神经元免受多种损伤。在皮摩尔浓度范围内,NAP通过与神经元直接相互作用提供神经保护。在飞摩尔浓度范围内,NAP需要胶质细胞的存在才能提供神经保护。为了进一步了解NAP提供神经保护的机制,人们寻找了特异性结合蛋白。微管蛋白是微管的主要亚基蛋白,被鉴定为一种NAP结合分子。NAP的结构允许其穿透细胞膜,随后与微管蛋白结合并促进微管组装,从而对星形胶质细胞起到细胞保护作用。NAP(10⁻¹⁵ M)在体外促进微管组装,并保护星形胶质细胞免受与微管破坏相关的锌中毒。用飞摩尔浓度的NAP孵育星形胶质细胞两小时,会导致微管重新组织以及免疫反应性非磷酸化tau蛋白短暂增加。微管是神经元和胶质细胞骨架的关键组成部分,调节细胞分裂、分化和保护,而tau蛋白病变是阿尔茨海默病和其他痴呆症的主要促成因素。这里描述的研究结果可能为神经保护化合物的研发开辟新的前景。

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