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眼镜蛇毒磷脂酶A2:对其作用于脂质/水界面的综述。

Cobra venom phospholipase A2: a review of its action toward lipid/water interfaces.

作者信息

Dennis E A, Darke P L, Deems R A, Kensil C R, Plückthun A

出版信息

Mol Cell Biochem. 1981 Apr 13;36(1):37-45. doi: 10.1007/BF02354830.

Abstract

This review focuses on the mechanism of action of phospholipase A2 from cobra venom (Naja naja naja) toward the lipid/water interface. Particular points of interest include dramatic changes in the enzyme activity if the physical state of its substrate is altered and the activation of the enzyme by phosphorylcholine containing lipids. The experimental findings include the following: Micellar substrates are hydrolyzed faster by the enzyme than various bilayer forms of substrate aggregation. The activity of the enzyme toward short chain phospholipids increases suddenly above their critical micelle concentrations. An abrupt change in susceptibility to the enzyme is observed at the thermotropic phase transition of phospholipid vesicles. The enzyme shows the kinetic phenomena of surface dilution and activation by certain lipids, which suggest a two-step mechanism of action. A model is discussed which accommodates the present data both for the action of this enzyme at various lipid/water interfaces as well as its interaction with synthetic monomeric ligands and substrates.

摘要

本综述聚焦于眼镜蛇毒(眼镜蛇)磷脂酶A2作用于脂质/水界面的作用机制。特别值得关注的要点包括:若改变其底物的物理状态,酶活性会发生显著变化;含磷脂酰胆碱的脂质可激活该酶。实验结果如下:与底物聚集的各种双层形式相比,胶束底物被该酶水解得更快。该酶对短链磷脂的活性在其临界胶束浓度以上会突然增加。在磷脂囊泡的热致相变时,观察到对该酶的敏感性发生突然变化。该酶表现出表面稀释和被某些脂质激活的动力学现象,这表明其作用机制为两步。文中讨论了一个模型,该模型既能解释该酶在各种脂质/水界面的作用,又能解释其与合成单体配体及底物的相互作用。

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