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Cell-surface insulin receptor cycling and its implication in the glycogenic response in cultured foetal hepatocytes.

机译:细胞表面胰岛素受体循环及其在胎儿肝细胞糖原反应中的意义。

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摘要

The insulin-receptor cycle was investigated in cultured foetal rat hepatocytes by determining the variations in insulin-binding sites at the cell surface after short exposure to the hormone. Binding of 125I-insulin was measured at 4 degrees C after dissociation of prebound native insulin. Two protocols were used: exchange binding assay and binding after acid treatment; both gave the same results. Cell-surface 125I-insulin-receptor binding decreased sharply (by 40%) during the first 5 min of 10 nM-insulin exposure (t1/2 = 2 min) and remained practically constant thereafter; subsequent removal of the hormone restored the initial binding within 10 min. This fall-rise sequence corresponded to variations in the number of insulin receptors at the cell surface, with no detectable change in receptor affinity. The reversible translocation of insulin receptors from the cell surface to a compartment not accessible to insulin at 4 degrees C was hormone-concentration- and temperature-dependent. SDS/polyacrylamide-gel electrophoresis after cross-linking of bound 125I-insulin to cell-surface proteins with disuccinimidyl suberate showed that these variations were not associated with changes in Mr of binding components, in particular for the major labelled band of Mr 130,000. The insulin-receptor cycle could be repeated after intermittent exposure to insulin. Continuous or intermittent exposure to the hormone gave a similar glycogenic response, contrary to the partial effect of a unique short (5-20 min) exposure. A relationship could be established between the repetitive character of the rapid insulin-receptor cycle and the maximal expression of the biological effect in cultured foetal hepatocytes.
机译:通过测定短暂暴露于激素后的细胞表面胰岛素结合位点的变化,对培养的胎鼠肝细胞中的胰岛素受体循环进行了研究。预结合的天然胰岛素解离后,在4摄氏度下测量125 I-胰岛素的结合。使用了两种方案:交换结合测定和酸处理后的结合。两者给出了相同的结果。细胞表面125 I-胰岛素受体的结合在10 nM胰岛素暴露的前5分钟(t1 / 2 = 2分钟)中急剧下降(下降40%),此后几乎保持恒定。随后去除激素可在10分钟内恢复初始结合。该下降序列对应于细胞表面胰岛素受体数目的变化,而受体亲和力没有可检测的变化。在4摄氏度时,胰岛素受体从细胞表面可逆转位至胰岛素无法接近的区室是激素浓度和温度依赖性的。用辛二酸二琥珀酰亚胺基酯将结合的125 I-胰岛素与细胞表面蛋白交联后的SDS /聚丙烯酰胺凝胶电泳显示,这些变化与结合成分的Mr改变无关,特别是对于130,000 Mr的主要标记带而言。间歇性接触胰岛素后,可以重复胰岛素受体循环。连续或间歇性暴露于激素会产生相似的糖原反应,这与独特的短暂(5-20​​分钟)暴露所产生的部分影响相反。在快速的胰岛素受体循环的重复特征与培养的胎儿肝细胞中生物学效应的最大表达之间可以建立关系。

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