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p185neu跨膜结构域的二聚化对于转化是必要的,但并不充分。

Dimerization of the p185neu transmembrane domain is necessary but not sufficient for transformation.

作者信息

Burke C L, Lemmon M A, Coren B A, Engelman D M, Stern D F

机构信息

Department of Pathology, Yale University School of Medicine, New Haven, Connecticut 06510, USA.

出版信息

Oncogene. 1997 Feb 13;14(6):687-96. doi: 10.1038/sj.onc.1200873.

Abstract

The neu proto-oncogene encodes a receptor tyrosine kinase (RTK). The oncogenic allele neu* (p185*) bears a glutamic acid for valine substitution at position 664 within the predicted transmembrane domain. We have used this mutant to explore the role of the transmembrane domain in signal transduction by RTKs. Analysis of a panel of neu* proteins with second-site mutations in the transmembrane domain revealed a strong correlation of dimerization with transformation. Both dimerization and transformation are dependent on a domain formed by the amino acids Val663-Glu664-Gly665 (VEG). However, movement of the VEG elsewhere within the transmembrane domain promoted weak dimerization but not transformation. Epidermal growth factor receptor (EGFR)/neu chimeras were used to determine if mutations that disrupt activation by Glu664 affect hormone-regulated signal transduction as well. These mutations (of Val663 and Gly665) did not affect regulation by EGF. Introduction of the known transmembrane dimerization domain from Glycophorin A (GpA) stimulated dimerization, but was not sufficient for transformation. These results indicate that dimerization is necessary but not sufficient for transforming activity. The homologous wild-type domain, VVG, is not required for hormone-regulated signaling.

摘要

神经原癌基因编码一种受体酪氨酸激酶(RTK)。致癌等位基因neu*(p185*)在预测的跨膜结构域内第664位的缬氨酸被谷氨酸取代。我们利用这种突变体来探究跨膜结构域在RTK信号转导中的作用。对一组在跨膜结构域有第二位点突变的neu*蛋白进行分析,发现二聚化与转化之间存在很强的相关性。二聚化和转化都依赖于由氨基酸Val663 - Glu664 - Gly665(VEG)形成的结构域。然而,VEG在跨膜结构域内其他位置的移动促进了弱二聚化,但没有促进转化。表皮生长因子受体(EGFR)/neu嵌合体被用于确定破坏由Glu664介导的激活的突变是否也会影响激素调节的信号转导。这些(Val663和Gly665的)突变不影响表皮生长因子(EGF)的调节作用。引入已知的来自血型糖蛋白A(GpA)的跨膜二聚化结构域可刺激二聚化,但不足以实现转化。这些结果表明,二聚化对于转化活性是必要的,但不是充分的。同源野生型结构域VVG对于激素调节的信号传导不是必需的。

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