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ErbB-3和ErbB-4分别作为所有Neu分化因子/神经调节蛋白亚型的低亲和力和高亲和力受体发挥作用。

ErbB-3 and ErbB-4 function as the respective low and high affinity receptors of all Neu differentiation factor/heregulin isoforms.

作者信息

Tzahar E, Levkowitz G, Karunagaran D, Yi L, Peles E, Lavi S, Chang D, Liu N, Yayon A, Wen D

机构信息

Department of Chemical Immunology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

J Biol Chem. 1994 Oct 7;269(40):25226-33.

PMID:7929212
Abstract

Neu differentiation factor (NDF or heregulin) elevates tyrosine phosphorylation of the ErbB-2 receptor tyrosine kinase, and it was, therefore, thought to function as a ligand of this receptor. However, several lines of evidence raised the possibility that the interaction between NDF and ErbB-2 involves another molecule, which belongs to the family of epidermal growth factor receptors. To address this question we constructed soluble chimeric proteins between alkaline phosphatase and the extracellular domains of ErbB-2 and either ErbB-3 or ErbB-4, two newly recognized members of the epidermal growth factor receptor family. Using the soluble proteins we found that beta isoforms of NDF specifically bind to the ErbB-3 and ErbB-4 receptors but not to the soluble ErbB-2 protein. When ectopically expressed in monkey fibroblasts, the full-length ErbB-3 and ErbB-4 receptors conferred specific binding to NDF. In these cells ErbB-3 displayed lower ligand binding affinity than ErbB-4, but like the latter receptor it preferred to bind the beta isoform over the alpha class of NDFs. These results indicate that both ErbB-3 and ErbB-4 function as physiological receptors of all NDF isoforms and suggest that a still unknown ligand of ErbB-2 exists.

摘要

神经分化因子(NDF,即这里的神经调节蛋白)可提高ErbB-2受体酪氨酸激酶的酪氨酸磷酸化水平,因此,它被认为是该受体的配体。然而,一些证据表明,NDF与ErbB-2之间的相互作用涉及另一种分子,该分子属于表皮生长因子受体家族。为了解决这个问题,我们构建了碱性磷酸酶与ErbB-2以及表皮生长因子受体家族两个新发现的成员ErbB-3或ErbB-4的胞外结构域之间的可溶性嵌合蛋白。利用这些可溶性蛋白,我们发现NDF的β亚型特异性结合ErbB-3和ErbB-4受体,但不与可溶性ErbB-2蛋白结合。当在猴成纤维细胞中异位表达时,全长的ErbB-3和ErbB-4受体赋予了对NDF的特异性结合。在这些细胞中,ErbB-3的配体结合亲和力低于ErbB-4,但与后者受体一样,它更倾向于结合NDF的β亚型而非α亚型。这些结果表明,ErbB-3和ErbB-4均作为所有NDF亚型的生理受体发挥作用,并提示存在一种仍未知的ErbB-2配体。

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