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Effects of covalently linked insulin dimers on receptor kinase activity and receptor down regulation

机译:共价连接的胰岛素二聚体对受体激酶活性和受体下调的影响

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>Certain covalently linked insulin dimers have previously been found to have a greater ability to bind to the insulin receptor than to stimulate lipogenesis in adipocytes. The present report presents data indicating that the same insulin dimers also have a greater ability to bind to the receptor than to stimulate the kinase activity of the insulin receptor. In particular, one such covalently linked insulin dimer had less than 1% the potency of native insulin in stimulating the receptor kinase although it could bind to the solubilized receptor with 30% the potency of native insulin. In contrast, this dimer could down regulate the insulin receptor with approximately 30% the potency of native insulin. These results suggest that stimulation of the receptor kinase may require more than simple occupancy of the receptor binding site whereas down regulation of the receptor may require only the binding of ligand to the receptor.
机译:先前已经发现某些共价连接的胰岛素二聚体具有比刺激脂肪细胞中的脂肪生成更大的结合胰岛素受体的能力。本报告提供的数据表明,与刺激胰岛素受体的激酶活性相比,相同的胰岛素二聚体还具有更大的结合受体的能力。特别地,一种这样的共价连接的胰岛素二聚体在刺激受体激酶上具有小于天然胰岛素效力的1%,尽管它可以以30%的天然胰岛素效力结合至溶解的受体。相反,该二聚体可能以天然胰岛素约30%的效力下调胰岛素受体。这些结果表明,刺激受体激酶可能需要的不仅仅是受体结合位点的简单占有,而受体的下调可能仅需要配体与受体的结合。

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