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Sprouty与Cbl之间直接相互作用的证据。

Evidence for direct interaction between Sprouty and Cbl.

作者信息

Wong E S, Lim J, Low B C, Chen Q, Guy G R

机构信息

Signal Transduction Laboratory, Institute of Molecular and Cell Biology, National University of Singapore, Singapore 117609, Singapore.

出版信息

J Biol Chem. 2001 Feb 23;276(8):5866-75. doi: 10.1074/jbc.M006945200. Epub 2000 Oct 26.

DOI:10.1074/jbc.M006945200
PMID:11053437
Abstract

Sprouty (SPRY) was first identified in a genetic screen in Drosophila as an antagonist of fibroblast and epidermal growth factor receptors and Sevenless signaling, seemingly by inhibiting the receptor tyrosine kinase (RTK)/Ras/MAPK pathway. To date, four mammalian Sprouty genes have been identified; the primary sequences of the gene products share a well conserved cysteine-rich C-terminal domain with their Drosophila counterpart. The N-terminal regions do not, however, exhibit a large degree of homology. This study was aimed at identifying proteins with which human SPRY2 (hSPRY2) interacts in an attempt to understand the mechanism by which Sprouty proteins exert their down-regulatory effects. Here, we demonstrate that hSPRY2 associates directly with c-Cbl, a known down-regulator of RTK signaling. A short sequence in the N terminus of hSPRY2 was found to bind directly to the Ring finger domain of c-Cbl. Parallel binding was apparent between the Drosophila homologs of Sprouty and Cbl, with cross-species associations occurring at least in vitro. Coexpression of hSPRY2 abrogated an increase in the rate of epidermal growth factor receptor internalization induced by c-Cbl, whereas a mutant hSPRY2 protein unable to bind c-Cbl showed no such effect. Our results suggest that one function of hSPRY2 in signaling processes downstream of RTKs may be to modulate c-Cbl physiological function such as that seen with receptor-mediated endocytosis.

摘要

Sprouty(SPRY)最初是在果蝇的基因筛选中被鉴定出来的,它作为成纤维细胞和表皮生长因子受体以及Sevenless信号的拮抗剂,似乎是通过抑制受体酪氨酸激酶(RTK)/Ras/MAPK途径来发挥作用。迄今为止,已鉴定出四个哺乳动物Sprouty基因;这些基因产物的一级序列与其果蝇对应物共享一个高度保守的富含半胱氨酸的C末端结构域。然而,N末端区域并没有表现出高度的同源性。本研究旨在鉴定与人类SPRY2(hSPRY2)相互作用的蛋白质,以试图了解Sprouty蛋白发挥其下调作用的机制。在此,我们证明hSPRY2直接与c-Cbl相关联,c-Cbl是一种已知的RTK信号下调因子。发现hSPRY2 N末端的一个短序列直接与c-Cbl的环指结构域结合。Sprouty和Cbl的果蝇同源物之间存在明显的平行结合关系,至少在体外存在跨物种关联。hSPRY2的共表达消除了由c-Cbl诱导的表皮生长因子受体内化速率的增加,而无法结合c-Cbl的突变型hSPRY2蛋白则没有这种作用。我们的结果表明,hSPRY2在RTK下游信号传导过程中的一个功能可能是调节c-Cbl的生理功能,例如在受体介导内吞作用中所观察到的功能。

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