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配体诱导的125I-表皮生长因子内化脱敏

Ligand-induced desensitization of 125I-epidermal growth factor internalization.

作者信息

Kuppuswamy D, Pike L J

机构信息

Howard Hughes Medical Institute, St. Louis, Missouri 63110.

出版信息

J Biol Chem. 1989 Feb 25;264(6):3357-63.

PMID:2492535
Abstract

The internalization of 125I-epidermal growth factor (EGF) by A431 cells was investigated. Control cells were able to internalize over 80% of receptor-bound 125I-EGF. By contrast, cells treated with EGF before incubation with 125I-EGF internalized only 50% of the surface-bound radioligand. The ligand-induced decrease in 125I-EGF internalization showed a dose response to EGF with half-maximal effect occurring at 3 nM. The alteration in the extent of 125I-EGF internalization did not require extended treatment with high concentrations of the hormone. When the internalization of picomolar versus nanomolar concentrations of EGF were compared, the lower concentrations of 125I-EGF were more completely internalized than the higher concentrations of radioligand. These data are consistent with the hypothesis that occupation of the EGF receptor by hormone rapidly leads to the activation of cellular processes which effectively desensitize the system to further ligand-induced internalization. The decrease in the extent of ligand internalization occurred in cells in which the protein kinase C (Ca2+/phospholipid-dependent enzyme) activity had been down-regulated by prolonged treatment with 12-O-tetradecanoyl-phorbol-13-acetate implying that the desensitization process is independent of protein kinase C. However, the effects of EGF on the extent of hormone internalization could be mimicked by the addition of A23187 and could be prevented by pretreatment of the cells with calmodulin antagonists suggesting the possibility that Ca2+-calmodulin is involved in the regulation of EGF receptor internalization in A431 cells.

摘要

研究了A431细胞对¹²⁵I-表皮生长因子(EGF)的内化作用。对照细胞能够内化超过80%与受体结合的¹²⁵I-EGF。相比之下,在用¹²⁵I-EGF孵育前先用EGF处理的细胞,仅内化了50%与表面结合的放射性配体。配体诱导的¹²⁵I-EGF内化减少呈现出对EGF的剂量反应,半数最大效应出现在3 nM。¹²⁵I-EGF内化程度的改变并不需要用高浓度激素进行长时间处理。当比较皮摩尔浓度与纳摩尔浓度的EGF的内化情况时,较低浓度的¹²⁵I-EGF比较高浓度的放射性配体更能被完全内化。这些数据与以下假设一致:激素占据EGF受体会迅速导致细胞过程的激活,从而有效地使系统对进一步的配体诱导内化产生脱敏作用。配体内化程度的降低发生在用12-O-十四烷酰佛波醇-13-乙酸酯长时间处理使蛋白激酶C(钙/磷脂依赖性酶)活性下调的细胞中,这意味着脱敏过程独立于蛋白激酶C。然而,EGF对激素内化程度的影响可通过添加A23187来模拟,并且可通过用钙调蛋白拮抗剂预处理细胞来防止,这表明Ca²⁺-钙调蛋白可能参与A431细胞中EGF受体内化的调节。

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