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黑曼巴蛇毒磷脂酶A2与单体底物类似物的相互作用。酶通过蛋白质-蛋白质或脂质-蛋白质相互作用激活?

Interaction of phospholipase A2 from Naja melanoleuca snake venom with monomeric substrate analogs. Activation of the enzyme by protein-protein or lipid-protein interactions?

作者信息

van Eijk J H, Verheij H M, Dijkman R, de Haas G H

出版信息

Eur J Biochem. 1983 Apr 15;132(1):183-8. doi: 10.1111/j.1432-1033.1983.tb07345.x.

Abstract

Unlike porcine pancreatic phospholipase A2, the enzyme from Naja melanoleuca does not display biphasic kinetic behaviour at substrate concentrations around the critical micelle concentration. This snake venom enzyme was further investigated by direct binding studies using n-tridecylphosphocholine. Binding of this substrate analog to the enzyme was monitored by using equilibrium gel filtration, equilibrium dialysis and ultraviolet difference spectroscopy. It is concluded that, in the presence of submicellar concentrations of n-tridecylphosphocholine, a lipid-protein complex is formed consisting of about 4 protein and 36 lipid molecules. Ca2+ ions are required for the formation of this complex. A model is proposed which describes the formation of this type of complex. These lipid-protein aggregates are held responsible for the non-hyperbolic kinetic behaviour of the snake venom enzyme towards monomeric substrates.

摘要

与猪胰磷脂酶A2不同,黑曼巴蛇的这种酶在临界胶束浓度附近的底物浓度下不会表现出双相动力学行为。通过使用正十三烷基磷胆碱的直接结合研究对这种蛇毒酶进行了进一步研究。通过平衡凝胶过滤、平衡透析和紫外差光谱法监测这种底物类似物与酶的结合。得出的结论是,在亚胶束浓度的正十三烷基磷胆碱存在下,会形成一种由约4个蛋白质分子和36个脂质分子组成的脂蛋白复合物。形成这种复合物需要Ca2+离子。提出了一个描述这种复合物形成的模型。这些脂蛋白聚集体被认为是蛇毒酶对单体底物呈现非双曲线动力学行为的原因。

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