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Structure-activity relationships of retinoids as inhibitors of calmodulin-dependent human erythrocyte Ca2+-ATPase activity and calmodulin binding to membranes

机译:类视黄醇作为钙调蛋白依赖性人红细胞Ca2 + -ATPase活性抑制剂和钙调蛋白与膜结合的结构活性关系

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pAll-trans retinoic acid displaces the binding of radiolabelled calmodulin to human erythrocyte membranes, and inhibits the activity of plasma membrane Ca(2+)-stimulated, Mg(2+)-dependent ATPase (Ca(2+)-ATPase; EC 3.6.1.3). This enzyme is dependent upon the action of calmodulin. In this study we explored the structural attributes of the retinoids which confer this ability to inhibit enzyme activity and calmodulin binding. With respect to the fatty acid side-chain, a clear requirement for inhibition is a trans-configuration of the polar end-group. The importance of the ring structure is indicated by the ineffectiveness of polyprenoic acid and a benzene ring retinoid analogue as inhibitors of enzyme activity and calmodulin binding. There was good correlation between the relative potencies of the analogues as enzyme inhibitors and as inhibitors of calmodulin binding. The ability of selected retinoid analogues, at physiological concentrations with respect to all-trans retinoic acid, to inhibit erythrocyte Ca(2+)-ATPase activity and membrane binding of calmodulin underscores the structurally specific effects of these compounds on the interaction of calmodulin with the membrane-bound enzyme./p
机译:>全反式维甲酸取代放射性标记的钙调蛋白与人类红细胞膜的结合,并抑制质膜Ca(2+)刺激的Mg(2+)依赖性ATPase(Ca(2 +)-ATPase ; EC 3.6.1.3)。该酶取决于钙调蛋白的作用。在这项研究中,我们探索了类维生素A的结构属性,这些属性赋予了这种抑制酶活性和钙调蛋白结合的能力。关于脂肪酸侧链,抑制的明确要求是极性端基的反式构型。环戊烯酸和苯环类视黄醇类似物作为酶活性和钙调蛋白结合抑制剂的无效性表明了环结构的重要性。作为酶抑制剂和钙调蛋白结合抑制剂的类似物的相对效力之间具有良好的相关性。选定的类维生素A类似物的能力,在相对于全反式维甲酸的生理浓度下,抑制红细胞Ca(2 +)-ATPase活性和钙调蛋白的膜结合,突显了这些化合物对钙调蛋白与钙调蛋白相互作用的结构特异性作用。膜结合酶。

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