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胰岛素对红细胞膜微粘度的调控

Control of erythrocyte membrane microviscosity by insulin.

作者信息

Dutta-Roy A K, Ray T K, Sinha A K

出版信息

Biochim Biophys Acta. 1985 Jun 11;816(1):187-90. doi: 10.1016/0005-2736(85)90408-0.

Abstract

The human erythrocyte membrane binds insulin through high-affinity, low-capacity binding sites (dissociation constant Kd1 2.45 X 10(-9)M; capacity n1 207 fmol/mg protein) and low-affinity, high-capacity binding sites (Kd2 0.63 X 10(-6) M; n2 37 pmol/mg protein). Treatment of the erythrocyte membrane or the intact cells with the physiological concentration of insulin, which is within the range of Kd value of the high-affinity sites, results in a significant reduction of the membrane microviscosity and the filtration time of the intact cells. Use of supraphysiological concentrations of the hormone reverses the effect of the lower concentration of insulin on the membrane microviscosity and the filtration time.

摘要

人类红细胞膜通过高亲和力、低容量结合位点(解离常数Kd1为2.45×10⁻⁹M;容量n1为207飞摩尔/毫克蛋白质)和低亲和力、高容量结合位点(Kd2为0.63×10⁻⁶M;n2为37皮摩尔/毫克蛋白质)结合胰岛素。用生理浓度的胰岛素处理红细胞膜或完整细胞,该浓度处于高亲和力位点的Kd值范围内,会导致膜微粘度和完整细胞过滤时间显著降低。使用超生理浓度的激素会逆转较低浓度胰岛素对膜微粘度和过滤时间的影响。

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