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谷氨酸脱羧酶和γ-氨基丁酸转氨酶的酶激活不可逆抑制剂在视网膜与大脑中的体内作用。

In vivo action of enzyme-activated irreversible inhibitors of glutamic acid decarboxylase and gamma-aminobutyric acid transaminase in retina vs. brain.

作者信息

Cubells J F, Blanchard J S, Smith D M, Makman M H

出版信息

J Pharmacol Exp Ther. 1986 Aug;238(2):508-14.

PMID:3735130
Abstract

The effects of low s.c. doses of gamma-acetylenic gamma-aminobutyric acid (GAG) on glutamic acid decarboxylase (GAD) and gamma-aminobutyric acid transaminase (GABA-T) activities, as well as of gamma-vinyl GABA (GVG) and gabaculine on GABA-T activities, were examined using preparations from retina and several other regions of rat central nervous system (CNS). GAG, in doses of 5 to 50 mg/kg, inactivated retinal GAD to a significantly greater degree than GAD from any other CNS region studied. Retinal GABA-T activities were also differentially inactivated by 1 to 50 mg/kg of GAG, 50 mg/kg of GVG, or 1 and 5 mg/kg of gabaculine. GAG, in doses of 25 and 50 mg/kg, more completely inactivated GAD and GABA-T in frontal cortex than in other brain regions. Frontal cortical GABA-T was not differentially inactivated by 10 and 50 mg/kg of GVG or 1 and 5 mg/kg of gabaculine. The effects of GAG on retinal GABA enzymes were long-lasting and not reversed by dialysis. The GAD and GABA-T activities from 1:1 mixes of control and GAG-treated retinal preparations were comparable to the means of the GAG-treated and control activities. The effects documented in this study, therefore, probably reflect irreversible in vivo changes. After peripheral administration, GAG, GVG and gabaculine might reach higher levels in the retina than in the brain. Alternatively, the differential effects of these compounds might be due to the relative proportions of catalytically active GABA enzymes in different CNS regions. On the basis of the foregoing results, the retina might be a particularly suitable region of the CNS for enzyme-activated irreversible inhibitors to label catalytically active enzymes of GABA metabolism.

摘要

采用大鼠中枢神经系统(CNS)视网膜及其他几个区域的组织制备物,研究了皮下注射低剂量的γ-乙炔基γ-氨基丁酸(GAG)对谷氨酸脱羧酶(GAD)和γ-氨基丁酸转氨酶(GABA-T)活性的影响,以及γ-乙烯基GABA(GVG)和加巴喷丁对GABA-T活性的影响。剂量为5至50mg/kg的GAG使视网膜GAD失活的程度明显高于所研究的任何其他CNS区域的GAD。1至50mg/kg的GAG、50mg/kg的GVG或1和5mg/kg的加巴喷丁也能使视网膜GABA-T活性产生不同程度的失活。剂量为25和50mg/kg的GAG使额叶皮质中的GAD和GABA-T失活比其他脑区更完全。10和50mg/kg的GVG或1和5mg/kg的加巴喷丁对额叶皮质GABA-T没有产生不同程度的失活作用。GAG对视网膜GABA酶的作用是持久的,且不能通过透析逆转。对照和经GAG处理的视网膜组织制备物按1:1混合后的GAD和GABA-T活性与经GAG处理和对照活性的平均值相当。因此,本研究中记录的作用可能反映了体内的不可逆变化。外周给药后,GAG、GVG和加巴喷丁在视网膜中的水平可能高于脑内。或者,这些化合物的不同作用可能是由于不同CNS区域中具有催化活性的GABA酶的相对比例不同。基于上述结果,视网膜可能是CNS中特别适合酶激活不可逆抑制剂标记GABA代谢中具有催化活性的酶的区域。

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