肝脏甘油激酶的一些特性及其与甘油利用调控的关系。

Some properties of hepatic glycerol kinase and their relation to the control of glycerol utilization.

作者信息

Robinson J, Newsholme E A

出版信息

Biochem J. 1969 May;112(4):455-64. doi: 10.1042/bj1120455.

DOI:10.1042/bj1120455

PMID:5801670

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1187733/

Abstract

Glycerol kinase (EC 2.7.1.30) is shown to catalyse a non-equilibrium reaction in rat liver; and, as it is the first enzyme in the pathway metabolizing glycerol, its properties may be pertinent to the metabolic regulation of glycerol uptake and utilization by this tissue. 2. The properties of hepatic glycerol kinase were studied by using a radiochemical technique to measure the enzyme activity. When the concentration of ATP is low the activity of glycerol kinase is inhibited by high concentrations of glycerol; but when the concentration of ATP is high there is no inhibition and the double-reciprocal plot is linear, providing a K(m) for glycerol of 3.16x10(-6)m. Glycerol kinase is activated by high ATP concentrations provided that the concentration of the second substrate (glycerol) is high; at low concentrations of glycerol ATP does not activate the enzyme so that the double-reciprocal plot is linear, providing a K(m) for ATP of 5.8x10(-5)m. It is suggested that these kinetics may be explained by a model similar to that described by Ferdinand (1966) for phosphofructokinase. 3. Hepatic glycerol kinase is inhibited by ADP and AMP, and raising the Mg(2+) concentration increases the inhibition by these two compounds; this suggests that ADP-Mg(2+) and AMP-Mg(2+) complexes are the inhibitory species. The physiological significance of these inhibitions may be to prevent phosphorylation of glycerol when the hepatic ATP concentration is low. It is suggested that this inhibition may provide an approach to the problem of measurement of rates of lipolysis by glycerol release in tissues that contain glycerol kinase (e.g. liver, kidney, muscle, adipose tissue). 4. Hepatic glycerol kinase is inhibited by l-3-glycerophosphate competitively with respect to glycerol. The physiological significance of this inhibition may be that factors that change the intracellular concentration of l-3-glycerophosphate could change glycerol uptake by the tissue. Thus it is suggested that thyroxine treatment or feeding rats on a diet high in glycerol, which increase the activity of glycerophosphate oxidase in liver and kidney cortex respectively, lead to an increased glycerol uptake through a decrease in the concentration of glycerophosphate in these tissues. It is known that ethanol administration decreases glycerol uptake by liver, and this can be explained by the increased concentration of l-3-glycerophosphate causing inhibition of glycerol kinase.

摘要

甘油激酶（EC 2.7.1.30）在大鼠肝脏中催化非平衡反应；由于它是甘油代谢途径中的首个酶，其特性可能与该组织对甘油摄取和利用的代谢调节相关。2. 采用放射化学技术测定酶活性，研究肝脏甘油激酶的特性。当ATP浓度较低时，高浓度甘油会抑制甘油激酶的活性；但当ATP浓度较高时，则不存在抑制作用，双倒数作图呈线性，得出甘油的米氏常数（K(m)）为3.16×10⁻⁶m。如果第二种底物（甘油）浓度较高，甘油激酶会被高浓度ATP激活；在甘油浓度较低时，ATP不会激活该酶，双倒数作图呈线性，得出ATP的K(m)为5.8×10⁻⁵m。有人认为，这些动力学可用类似于Ferdinand（1966年）描述磷酸果糖激酶的模型来解释。3. 肝脏甘油激酶受ADP和AMP抑制，提高Mg²⁺浓度会增强这两种化合物的抑制作用；这表明ADP-Mg²⁺和AMP-Mg²⁺复合物是抑制性物质。这些抑制作用的生理意义可能是在肝脏ATP浓度较低时防止甘油磷酸化。有人认为，这种抑制作用可能为解决通过含甘油激酶的组织（如肝脏、肾脏、肌肉、脂肪组织）中甘油释放来测量脂肪分解速率的问题提供一种方法。4. 肝脏甘油激酶受l-3-磷酸甘油相对于甘油的竞争性抑制。这种抑制作用的生理意义可能是，改变细胞内l-3-磷酸甘油浓度的因素可能会改变组织对甘油的摄取。因此有人认为，甲状腺素处理或用富含甘油的饲料喂养大鼠，分别会增加肝脏和肾皮质中磷酸甘油氧化酶的活性，通过降低这些组织中磷酸甘油的浓度导致甘油摄取增加。已知给予乙醇会降低肝脏对甘油的摄取，这可以用l-3-磷酸甘油浓度增加导致甘油激酶受抑制来解释。