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神经分化因子/神经调节蛋白受体ErbB-3和ErbB-4的差异表达及其在抑制神经元分化中的作用。

Differential expression of NDF/neuregulin receptors ErbB-3 and ErbB-4 and involvement in inhibition of neuronal differentiation.

作者信息

Pinkas-Kramarski R, Eilam R, Alroy I, Levkowitz G, Lonai P, Yarden Y

机构信息

Department of Molecular Cell Biology, The Weizmann Institute of Science, Rehovot, Israel.

出版信息

Oncogene. 1997 Dec 4;15(23):2803-15. doi: 10.1038/sj.onc.1201466.

DOI:10.1038/sj.onc.1201466
PMID:9419971
Abstract

Two receptor tyrosine kinases, ErB-3 and ErbB-4, mediate signaling by Neu differentiation factors (NDFs, also called neuregulins), while ErbB-1 and ErbB-2 serve as co-receptors. We show that the two NDF/neuregulin receptors differ in spatial and temporal expression patterns: The kinase-defective receptor, ErbB-3, is expressed primarily in epithelial layers of various organs, in the peripheral nervous system, and in adult brain, whereas ErbB-4 is restricted to the developing central nervous system and to the embryonic heart. An example of alternating expression of the two receptors is provided by the developing cerebellum: During postnatal cerebellar development, ErbB-4 expression slightly decreases along with a decline in NDF transcription, whereas ErbB-3 expression commences after the peak of neurogenesis. To study functional differences, we established primary brain cultures and found that ErbB-3 was expressed only in oligodendrocytes, whereas ErbB-4 expression was shared by oligodendrocytes, astrocytes and neurons. Blocking the action of endogenous NDF in vitro, by using a soluble form of ErbB-4, accelerated neurite outgrowth in both primary cultures and in neuronal-type cultures of the P19 teratocarcinoma, suggesting an inhibitory effect of NDF on neural differentiation. Apparently, ErbB-3 is associated with proliferation of P19 cells, whereas ErbB-4 correlates with a differentiated phenotype. We conclude that the two NDF receptors play distinct, rather than redundant, developmental and physiological roles.

摘要

两种受体酪氨酸激酶,ErB-3和ErbB-4,介导神经分化因子(NDFs,也称为神经调节蛋白)的信号传导,而ErbB-1和ErbB-2作为共受体。我们发现这两种NDF/神经调节蛋白受体在空间和时间表达模式上存在差异:激酶缺陷型受体ErB-3主要在各种器官的上皮层、外周神经系统和成年大脑中表达,而ErbB-4则局限于发育中的中枢神经系统和胚胎心脏。发育中的小脑提供了这两种受体交替表达的一个例子:在出生后小脑发育过程中,ErbB-4的表达随着NDF转录的下降而略有降低,而ErbB-3的表达在神经发生高峰后开始。为了研究功能差异,我们建立了原代脑培养物,发现ErB-3仅在少突胶质细胞中表达,而ErbB-4的表达则少突胶质细胞、星形胶质细胞和神经元共有。通过使用可溶性形式的ErbB-4在体外阻断内源性NDF的作用,加速了原代培养物和P19畸胎瘤神经元型培养物中的神经突生长,表明NDF对神经分化有抑制作用。显然,ErB-3与P19细胞的增殖有关,而ErbB-4与分化表型相关。我们得出结论,这两种NDF受体在发育和生理过程中发挥着不同而非冗余的作用。

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