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从年轻和衰老的WI-38细胞分离的质膜中表皮生长因子受体的表皮生长因子依赖性磷酸化。

EGF-dependent phosphorylation of the EGF receptor in plasma membranes isolated from young and senescent WI-38 cells.

作者信息

Brooks K M, Phillips P D, Carlin C R, Knowles B B, Cristofalo V J

机构信息

Wistar Institute of Anatomy and Biology, Philadelphia, Pennsylvania 19104.

出版信息

J Cell Physiol. 1987 Dec;133(3):523-31. doi: 10.1002/jcp.1041330313.

Abstract

Tyrosine-specific phosphorylation of the receptor for epidermal growth factor (EGF) in plasma membranes isolated from WI-38 cells is EGF-dependent and occurs to an equivalent extent and on identical tryptic peptides in preparations from cells of various in vitro ages. There is a marked reduction, however, in phosphorylation of receptor molecules from senescent as compared with young WI-38 cells, if enzyme activity is assayed in an immune complex following solubilization of plasma membranes with Nonidet P-40 (NP-40). Differences in the level of receptor phosphorylation in young vs. senescent NP-40 extracts are not resolved by changing the temperature at which the assay is performed, or the length of incubation. Moreover, addition of NP-40 or chloroform-methanol extracts of young cells to assays measuring receptor phosphorylation in senescent cell NP-40 preparations does not augment the senescent enzyme activity. The immunopurified senescent receptor is, however, capable of catalyzing phosphorylation of exogenous substrates. These results indicate that the loss of receptor autophosphorylation in solubilized preparations may result from a differential sensitivity of the senescent cell receptor to the detergent. This finding provides a marker for senescence and suggests subtle changes in protein structure, conformation, or regulation of the EGF receptor in senescent cells.

摘要

从WI-38细胞分离的质膜中,表皮生长因子(EGF)受体的酪氨酸特异性磷酸化是依赖于EGF的,并且在来自不同体外培养龄期细胞的制剂中,其发生程度相同且作用于相同的胰蛋白酶肽段。然而,如果在用诺乃洗涤剂P-40(NP-40)溶解质膜后,在免疫复合物中测定酶活性,与年轻的WI-38细胞相比,衰老细胞中受体分子的磷酸化会显著降低。通过改变测定时的温度或孵育时间,不能消除年轻与衰老NP-40提取物中受体磷酸化水平的差异。此外,将年轻细胞的NP-40或氯仿 - 甲醇提取物添加到衰老细胞NP-40制剂中测量受体磷酸化的测定中,并不会增强衰老细胞的酶活性。然而,免疫纯化的衰老受体能够催化外源底物的磷酸化。这些结果表明,溶解制剂中受体自身磷酸化的丧失可能是由于衰老细胞受体对去污剂的敏感性不同所致。这一发现为衰老提供了一个标志物,并提示衰老细胞中EGF受体的蛋白质结构、构象或调节存在细微变化。

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