首页> 美国卫生研究院文献>Biochemical Journal >Dependence of in vivo glutamine synthetase activity on ammonia concentration in rat brain studied by 1H - 15N heteronuclear multiple-quantum coherence-transfer NMR.
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Dependence of in vivo glutamine synthetase activity on ammonia concentration in rat brain studied by 1H - 15N heteronuclear multiple-quantum coherence-transfer NMR.

机译:通过1H-15N异核多量子相干转移NMR研究了体内谷氨酰胺合成酶活性对大鼠脑中氨浓度的依赖性。

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摘要

The dependence of the in vivo rate of glutamine synthesis on the substrate ammonia concentration was studied in rat brain by 1H-15N heteronuclear multiple-quantum coherence-transfer NMR in combination with biochemical techniques. In vivo rates were measured at various steady-state blood and brain ammonia concentrations within the ranges 0.4-0.55 mumol/g and 0.86-0.98 mumol/g respectively, after low-rate intravenous 15NH4+ infusion (isotope chase). The rate of glutamine synthesis at steady state was determined from the change in brain [5-15N]glutamine levels during isotope chase, observed selectively through the amide proton by NMR, and 15N enrichments of brain glutamine and of blood and brain ammonia measured byN gas chromatography-MS. The in vivo rate (v) was 3.3-4.5 mumol/h per g of brain at blood ammonia concentrations (s) of 0.40-0.55 mumol/g. A linear increase of 1/v with 1/s permitted estimation of the in vivo glutamine synthetase (GS) activity at a physiological blood ammonia concentration to be 0.4-2.1 mumol/h per g. The observed ammonia-dependence strongly suggests that, under physiological conditions, in vivo GS activity is kinetically limited by sub-optimal in situ concentrations of ammonia as well as glutamate and ATP. Comparison of the observed in vivo GS activity with the reported in vivo rates of glutaminase and of gamma-aminobutyrate (GABA) synthesis suggests that, under mildly hyperammonaemic conditions, glutamine is synthesized at a sufficiently high rate to serve as a precursor of GABA, but glutaminase-catalysed hydrolysis of glutamine is too slow to be the sole provider of glutamate used for GABA synthesis.
机译:通过1H-15N异核多量子相干转移NMR结合生化技术研究了大鼠脑中谷氨酰胺合成的体内速率对底物氨浓度的依赖性。在低速静脉内15NH4 +输注(追逐同位素)后,分别在0.4-0.55μmol/ g和0.86-0.98μmol/ g范围内的各种稳态血液和脑氨浓度下测量体内率。稳定状态下谷氨酰胺的合成速率由同位素追踪过程中脑中[5-15N]谷氨酰胺水平的变化确定,该变化通过NMR通过酰胺质子选择性观察到,并由N气体测定了15N富集的脑谷氨酰胺以及血液和脑氨色谱-MS。在血氨浓度为0.40-0.55μmol/ g的情况下,体内速率(v)为每g脑3.3-4.5μmol/ h。以1 / s线性增加1 / v,可以估计在生理性血氨浓度为0.4-2.1μmol/ h / g的情况下体内谷氨酰胺合成酶(GS)活性。观察到的氨依赖性强烈表明,在生理条件下,体内GS活性在动力学上受到亚最佳浓度的氨,谷氨酸和ATP的动力学限制。将观察到的体内GS活性与报道的体内谷氨酰胺酶和γ-氨基丁酸(GABA)合成的体内速率进行比较,结果表明,在轻度高氨血症的条件下,谷氨酰胺的合成速率足够高,可以用作GABA的前体。谷氨酰胺酶催化的谷氨酰胺水解太慢,以致于不能单独提供用于GABA合成的谷氨酸。

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