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抗胰岛素抗体对胰岛素结合及生物活性的调节:与受体自身聚集在激素作用中可能发挥的作用的关系。

Modulation of binding and bioactivity of insulin by anti-insulin antibody: relation to possible role of receptor self-aggregation in hormone action.

作者信息

Shechter Y, Chang K J, Jacobs S, Cuatrecasas P

出版信息

Proc Natl Acad Sci U S A. 1979 Jun;76(6):2720-4. doi: 10.1073/pnas.76.6.2720.

Abstract

Incubation of physiological concentrations of 125I-labeled insulin with liver membranes in the presence of anti-insulin IgG results in a 7- to 15-fold increase in the specific binding of the hormone. The low-affinity/high-capacity binding sites are replaced by an apparently homogeneous class of high-affinity sites, and the nonlinear Scatchard plots are converted to linear plots without a change in the maximum number of binding sites. Similarly, the binding of insulin to receptors in 3T3 fibroblasts is increased substantially in the presence of anti-insulin antibody, and the biological activity of subactive concentrations of insulin is enhanced by antibody in these cells. However, the affinity of 125I-labeled epidermal growth factors (EGF) in fibroblasts is not affected by anti-EGF IgG. In adipocytes anti-insulin IgG in the same concentration range only inhibits the binding of insulin and suppresses insulin-mediated glucose oxidation. Monovalent Fab' fragments from anti-insulin IgG inhibit the binding of the hormone, indicating that the enhancement of binding in liver membranes and fibroblasts requires the bivalency of the antibody.

摘要

在抗胰岛素IgG存在的情况下,将生理浓度的125I标记胰岛素与肝细胞膜一起孵育,会使该激素的特异性结合增加7至15倍。低亲和力/高容量结合位点被一类明显均一的高亲和力位点所取代,非线性的Scatchard图转变为线性图,而结合位点的最大数量没有变化。同样,在抗胰岛素抗体存在的情况下,胰岛素与3T3成纤维细胞中受体的结合显著增加,并且在这些细胞中,亚活性浓度胰岛素的生物活性被抗体增强。然而,成纤维细胞中125I标记的表皮生长因子(EGF)的亲和力不受抗EGF IgG的影响。在脂肪细胞中,相同浓度范围内的抗胰岛素IgG仅抑制胰岛素的结合并抑制胰岛素介导的葡萄糖氧化。抗胰岛素IgG的单价Fab′片段抑制该激素的结合,表明肝细胞膜和成纤维细胞中结合的增强需要抗体的二价性。

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Modulation of Gonadotropins Activity by Antibodies.抗体对促性腺激素活性的调节
Front Endocrinol (Lausanne). 2019 Feb 18;10:15. doi: 10.3389/fendo.2019.00015. eCollection 2019.
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Insulin does not aggregate its own receptor.胰岛素不会使自身受体聚集。
Diabetologia. 1983 Apr;24(4):304-5. doi: 10.1007/BF00282720.

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