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神经调节蛋白与神经胶质瘤中的ErbB-2/3/4受体

Heregulins and the ErbB-2/3/4 receptors in gliomas.

作者信息

Westphal M, Meima L, Szonyi E, Lofgren J, Meissner H, Hamel W, Nikolics K, Sliwkowski M X

机构信息

Department of Neurosurgery, University Hospital Eppendorf, Hamburg, Germany.

出版信息

J Neurooncol. 1997 Dec;35(3):335-46. doi: 10.1023/a:1005837122181.

Abstract

The activation of autocrine loops involving proto-oncogene related receptor tyrosine kinases has led to the analysis of a large number of growth factor systems in human glioma specimens and cell lines. The ErbB-2 system, also called HER-2 or neu, is analogous to the epidermal growth factor receptor system (EGF-R, ErbB-1). Neuregulins consist of a large family of proteins arising from alternative mRNA splicing of a single gene located at 8p22-p11. Activation of ErbB-2 by neuregulins occurs in heterodimeric complexes with ErbB-3 and ErbB-4. A panel of human glioma cell lines, which had previously been analyzed for ErbB-2 expression, was examined for ErbB-3 and ErbB-4 expression. Coordinate expression of ErbB-2, -3 or -4 was not observed in these cell lines. Despite the presence of a complete system capable of signaling in about half the cell lines, no constitutive activation of ErbB-2, -3 or -4 was observed, and autophosphorylation of ErbB-2 in response to heregulin was observed only in one cell line from the panel, NCE-G84. Moreover, the addition of recombinant heregulin or antibodies capable of disrupting ErbB-2/ErbB-3 complexes had no effect on cell proliferation. We conclude that the role of neuregulins and its receptors in the control of glioma cell proliferation may be limited or may be context dependent on in situ conditions which are lost in vitro. Alternatively, neuregulins may be involved in cell differentiation or survival in the central nervous system. Data supporting these conclusions are described in more detail herein.

摘要

涉及原癌基因相关受体酪氨酸激酶的自分泌环激活,促使人们对人类胶质瘤标本和细胞系中的大量生长因子系统进行分析。ErbB-2系统,也称为HER-2或neu,类似于表皮生长因子受体系统(EGF-R,ErbB-1)。神经调节蛋白由一大类蛋白质组成,这些蛋白质源于位于8p22-p11的单个基因的可变mRNA剪接。神经调节蛋白对ErbB-2的激活发生在与ErbB-3和ErbB-4形成的异二聚体复合物中。对一组先前已分析过ErbB-2表达的人类胶质瘤细胞系进行了ErbB-3和ErbB-4表达检测。在这些细胞系中未观察到ErbB-2、-3或-4的协同表达。尽管约一半的细胞系中存在完整的信号传导系统,但未观察到ErbB-2、-3或-4的组成性激活,仅在该组中的一个细胞系NCE-G84中观察到ErbB-2对这里调节蛋白的自磷酸化。此外,添加重组这里调节蛋白或能够破坏ErbB-2/ErbB-3复合物的抗体对细胞增殖没有影响。我们得出结论,神经调节蛋白及其受体在控制胶质瘤细胞增殖中的作用可能有限,或者可能取决于体外培养中丢失的原位条件。或者,神经调节蛋白可能参与中枢神经系统的细胞分化或存活。本文将更详细地描述支持这些结论的数据。

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