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首页> 外文期刊>Molecular and Cellular Biology >Transcriptional activation and transformation by FosB protein require phosphorylation of the carboxyl-terminal activation domain.
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Transcriptional activation and transformation by FosB protein require phosphorylation of the carboxyl-terminal activation domain.

机译:FosB蛋白的转录激活和转化需要羧基末端激活域的磷酸化。

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摘要

The transcription factor AP-1, composed of Fos-Jun dimers, mediates some aspects of the cellular response to growth factors. Transcriptional activation and neoplastic transformation by FosB, a member of the Fos family of proteins, require the presence of a potent C-terminal activation domain. Here we show by mutational analysis that the FosB C-terminal domain has a proline-based motif that is essential for both of these functions. Phosphopeptide mapping experiments show that the C terminus of FosB is phosphorylated within a cluster of functionally redundant serine residues that is adjacent to this proline-based motif. Mutation of these serine residues to alanine severely reduces the ability of this region to function as an activation domain and inhibits the ability of FosB protein to function as a transforming protein. Several observations suggest that the kinase responsible for phosphorylation of these sites is distinct from the mitogen-activation protein kinases and stress-activated protein kinases. Our results show that transcriptional activation and neoplastic transformation by the FosB protein are dependent on phosphorylation within the C terminus. This form of control may provide a potential mechanism of signal integration at the level of a single transcription factor.
机译:由Fos-Jun二聚体组成的转录因子AP-1介导细胞对生长因子的某些反应。 FosB(Fos蛋白家族的成员)的转录激活和肿瘤转化需要有效的C端激活域存在。在这里,我们通过突变分析表明,FosB C末端域具有基于脯氨酸的基序,这对于这两个功能都是必不可少的。磷酸肽图实验表明,FosB的C末端在与该基于脯氨酸的基序相邻的功能丰富的丝氨酸残基簇中被磷酸化。这些丝氨酸残基突变为丙氨酸会严重降低该区域充当激活域的能力,并抑制FosB蛋白充当转化蛋白的能力。几个观察结果表明,负责这些位点磷酸化的激酶不同于促分裂原活化蛋白激酶和应激活化蛋白激酶。我们的结果表明,FosB蛋白的转录激活和肿瘤转化取决于C末端的磷酸化。这种控制形式可以在单个转录因子水平上提供信号整合的潜在机制。

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