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神经分化因子刺激Sp1转录因子的磷酸化和激活。

Neu differentiation factor stimulates phosphorylation and activation of the Sp1 transcription factor.

作者信息

Alroy I, Soussan L, Seger R, Yarden Y

机构信息

Department of Biological Regulation, The Weizmann Institute of Science, Rehovot 76100, Israel.

出版信息

Mol Cell Biol. 1999 Mar;19(3):1961-72. doi: 10.1128/MCB.19.3.1961.

Abstract

Neu differentiation factors (NDFs), or neuregulins, are epidermal growth factor-like growth factors which bind to two tyrosine kinase receptors, ErbB-3 and ErbB-4. The transcription of several genes is regulated by neuregulins, including genes encoding specific subunits of the acetylcholine receptor at the neuromuscular junction. Here, we have examined the promoter of the acetylcholine receptor epsilon subunit and delineated a minimal CA-rich sequence which mediates transcriptional activation by NDF (NDF-response element [NRE]). Using gel mobility shift analysis with an NRE oligonucleotide, we detected two complexes that are induced by treatment with neuregulin and other growth factors and identified Sp1, a constitutively expressed zinc finger phosphoprotein, as a component of one of these complexes. Phosphatase treatment, two-dimensional gel electrophoresis, and an in-gel kinase assay indicated that Sp1 is phosphorylated by a 60-kDa kinase in response to NDF-induced signals. Moreover, Sp1 seems to act downstream of all members of the ErbB family and thus may funnel the signaling of the ErbB network into the nucleus.

摘要

神经分化因子(NDFs),即神经调节蛋白,是一类表皮生长因子样生长因子,可与两种酪氨酸激酶受体ErbB-3和ErbB-4结合。神经调节蛋白可调控多个基因的转录,包括编码神经肌肉接头处乙酰胆碱受体特定亚基的基因。在此,我们研究了乙酰胆碱受体ε亚基的启动子,并确定了一个最小的富含CA的序列,该序列介导NDF的转录激活作用(NDF反应元件 [NRE])。通过用NRE寡核苷酸进行凝胶迁移率变动分析,我们检测到两种受神经调节蛋白和其他生长因子处理诱导的复合物,并鉴定出一种组成型表达的锌指磷蛋白Sp1是其中一种复合物的成分。磷酸酶处理、二维凝胶电泳和凝胶内激酶分析表明,Sp1会响应NDF诱导的信号而被一种60 kDa的激酶磷酸化。此外,Sp1似乎在ErbB家族所有成员的下游起作用,因此可能将ErbB网络的信号导入细胞核。

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