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由谷氨酰胺形成细胞外谷氨酸:排除焦谷氨酸作为中间产物。

Formation of extracellular glutamate from glutamine: exclusion of pyroglutamate as an intermediate.

作者信息

Mena Fernando V, Baab Peter J, Zielke Carol L, Huang Yinyin, Zielke H Ronald

机构信息

Department of Pediatrics, University of Maryland School of Medicine, Bressler Research Building, Room 10-035, 655 West Baltimore Street, Baltimore, MD 21201-1559, USA.

出版信息

Brain Res. 2005 Aug 2;1052(1):88-96. doi: 10.1016/j.brainres.2005.06.014.

Abstract

A 4.6-fold increase in interstitial glutamate was observed following the reverse microdialysis of 5 mM glutamine into the rat hippocampus. Two possible mechanisms of glutamine hydrolysis were examined: (a) an enzymatic glutaminase activity and (b) a non-enzymatic mechanism. Injection of 14C-glutamine at the site of microdialysis followed by microdialysis with artificial cerebral spinal fluid allowed isolation of 14C-glutamine (63%), 14C-glutamate (14%), and a compound tentatively identified as pyroglutamate (22%). In this study, we determined if non-enzymatic pyroglutamate formation from glutamine contributed to the synthesis of glutamate. Pyroglutamate is in chemical equilibrium with glutamate, although under physiological conditions, the chemical equilibrium is strongly in the direction of pyroglutamate. In vitro stability studies indicated that 14C-glutamine and 14C-pyroglutamate are not subject to significant non-enzymatic breakdown at pH 6.5-7.5 at 37 degrees C for up to 8 h. Reverse microdialysis with 1 mM pyroglutamate did not increase interstitial glutamate levels. Following injection of 14C-pyroglutamate and microdialysis, radioactivity was recovered in 14C-pyroglutamate (88%) and 14C-glutamine (11%). Less than 1% of the radioactivity was recovered as glutamate. Our data do not support a role of pyroglutamate as an intermediate in the formation of extracellular glutamate following the infusion of glutamine. However, it confirms that pyroglutamate, a known constituent in brain, is actively metabolized in brain cells and contributes to glutamine in the interstitial space.

摘要

将5 mM谷氨酰胺反向微透析入大鼠海马体后,观察到间质谷氨酸增加了4.6倍。研究了谷氨酰胺水解的两种可能机制:(a) 谷氨酰胺酶活性和(b) 非酶促机制。在微透析部位注射14C-谷氨酰胺,然后用人工脑脊液进行微透析,分离出14C-谷氨酰胺(63%)、14C-谷氨酸(14%)和一种暂定为焦谷氨酸的化合物(22%)。在本研究中,我们确定谷氨酰胺非酶促形成焦谷氨酸是否有助于谷氨酸的合成。焦谷氨酸与谷氨酸处于化学平衡状态,尽管在生理条件下,化学平衡强烈倾向于焦谷氨酸。体外稳定性研究表明,14C-谷氨酰胺和14C-焦谷氨酸在37℃、pH 6.5 - 7.5条件下长达8小时不会发生显著的非酶促分解。用1 mM焦谷氨酸进行反向微透析不会增加间质谷氨酸水平。注射14C-焦谷氨酸并进行微透析后,放射性在14C-焦谷氨酸(88%)和14C-谷氨酰胺(11%)中回收。回收的放射性中作为谷氨酸的不到1%。我们的数据不支持焦谷氨酸在输注谷氨酰胺后作为细胞外谷氨酸形成中间体的作用。然而,它证实了焦谷氨酸作为大脑中的一种已知成分,在脑细胞中被积极代谢,并有助于间质空间中的谷氨酰胺形成。

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