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首页> 外文期刊>Cellular Signalling >The Shp-1 and Shp-2, tyrosine phosphatases, are recruited on cell membrane in two distinct molecular complexes including Ret oncogenes
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The Shp-1 and Shp-2, tyrosine phosphatases, are recruited on cell membrane in two distinct molecular complexes including Ret oncogenes

机译:Shp-1和Shp-2,酪氨酸磷酸酶被募集到细胞膜上的两个不同分子复合物中,包括Ret癌基因

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摘要

The Shp-2 and Shp-1 non-transmembrane tyrosine phosphatases display different and even opposing effects on downstream signaling events initiated by Ret activation. By using rat pheochromocytoma-derived PC 12 cells, here we studied the interactions of Shp-2 and Shp-1 with two activated mutants of Ret receptor, Ret(C634Y) and Ret(M918T). Each of these mutated receptors causes inheritance of distinct cancer syndromes, multiple endocrine neoplasia (MEN) type 2A and type 2B, respectively.We show that: (i) both Shp-1 and Shp-2 are associated to a multiprotein complex that includes Ret mutants; (ii) the Shp-1-Ret complexes are distinct from Shp-2-Ret complexes, and these complexes are differently distributed inside and outside lipid rafts; (iii) constitutively activated Ret proteins neither directly bind to nor are substrates of these phosphatases. Our results well support the evidence that Ret complexes within and outside rafts mediate distinct biological functions, and indicate that the presence of either Slips participates to determine such functions. (C) 2004 Elsevier Inc. All rights reserved.
机译:Shp-2和Shp-1非跨膜酪氨酸磷酸酶对Ret激活引发的下游信号转导事件表现出不同甚至相反的影响。通过使用大鼠嗜铬细胞瘤衍生的PC 12细胞,我们研究了Shp-2和Shp-1与Ret受体的两个活化突变体Ret(C634Y)和Ret(M918T)的相互作用。这些突变受体中的每一个都分别导致不同的癌症综合征,2A型和2B型多发性内分泌肿瘤(MEN)的遗传。我们证明:(i)Shp-1和Shp-2都与包含Ret的多蛋白复合物相关突变体(ii)Shp-1-Ret复合物不同于Shp-2-Ret复合物,并且这些复合物在脂质筏的内部和外部分布不同; (iii)组成型活化的Ret蛋白既不直接结合也不是这些磷酸酶的底物。我们的结果很好地支持了筏内部和外部的Ret复合物介导不同生物学功能的证据,并表明任一条滑道的存在都参与了此类功能的确定。 (C)2004 Elsevier Inc.保留所有权利。

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