首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Detection of glutamine synthetase in the cerebrospinal fluid of Alzheimer diseased patients: a potential diagnostic biochemical marker.
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Detection of glutamine synthetase in the cerebrospinal fluid of Alzheimer diseased patients: a potential diagnostic biochemical marker.

机译:阿尔茨海默病患者脑脊液中谷氨酰胺合成酶的检测:潜在的诊断生化标记。

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摘要

In this report, 8- and 2-azidoadenosine 5'-[gamma-32P]triphosphate were used to examine cerebrospinal fluid (CSF) samples for the presence of an ATP binding protein unique to individuals with Alzheimer disease (AD). A 42-kDa ATP binding protein was found in the CSF of AD patients that is not observed in CSF from normal patients or other neurological controls. The photolabeling is saturated with 30 microM 2-azidoadenosine 5'-[gamma-32P]triphosphate. Photoinsertion can be totally prevented by the addition of 25 microM ATP. Photoinsertion of 2-azidoadenosine 5'-triphosphate into the protein is only weakly protected by other nucleotides such as ADP and GTP, indicating that this is a specific ATP binding protein. A total of 83 CSF samples were examined in a blind manner. The 42-kDa protein was detected in 38 of 39 AD CSF samples and in only 1 of 44 control samples. This protein was identified as glutamine synthetase [GS; glutamate-ammonia ligase; L-glutamate:ammonia ligase (ADP-forming), EC 6.3.1.2] based on similar nucleotide binding properties, comigration on two-dimensional gels, reaction with a polyclonal anti-GS antibody, and the presence of significant GS enzyme activity in AD CSF. In brain, GS plays a key role in elimination of free ammonia and also converts the neurotransmitter and excitotoxic amino acid glutamate to glutamine, which is not neurotoxic. The involvement of GS, if any, in the onset of AD is unknown. However, the presence of GS in the CSF of terminal AD patients suggests that this enzyme may be a useful diagnostic marker and that further study is warranted to determine any possible role for glutamate metabolism in the pathology of AD.
机译:在此报告中,使用了8和2-叠氮腺苷5'-[γ-32P]三磷酸来检查脑脊髓液(CSF)样品中是否存在阿尔茨海默病(AD)个体所特有的ATP结合蛋白。在AD患者的CSF中发现了42 kDa ATP结合蛋白,而在正常患者或其他神经系统对照的CSF中未观察到。用30 microM 2-叠氮腺苷5'-[γ-32P]三磷酸饱和光标记。添加25 microM ATP可以完全防止光插入。将2-叠氮腺苷5'-三磷酸光插入该蛋白质仅受到其他核苷酸(例如ADP和GTP)的弱保护,这表明这是一种特异性的ATP结合蛋白。盲法检查了总共83个CSF样品。在39个AD CSF样品中的38个和44个对照样品中仅1个中检测到42 kDa蛋白。该蛋白被鉴定为谷氨酰胺合成酶[GS; G.N。谷氨酸氨连接酶; L-谷氨酸:氨连接酶(形成ADP),EC 6.3.1.2],基于相似的核苷酸结合特性,在二维凝胶上进行迁移,与多克隆抗GS抗体反应以及AD中存在明显的GS酶活性脑脊液。在脑中,GS在消除游离氨中起关键作用,还将神经递质和兴奋性氨基酸谷氨酸转化为无神经毒性的谷氨酰胺。尚不清楚GS是否与AD发作有关。然而,晚期AD患者的CSF中存在GS提示该酶可能是有用的诊断标志物,因此有必要进行进一步的研究以确定谷氨酸代谢在AD病理中的任何可能作用。

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