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碱性螺旋-环-螺旋(bHLH)转录因子Atoh8的转录活性特征分析

Characterization of the transcriptional activity of the basic helix-loop-helix (bHLH) transcription factor Atoh8.

作者信息

Ejarque Miriam, Altirriba Jordi, Gomis Ramon, Gasa Rosa

机构信息

Diabetes and Obesity Research Laboratory, Institut D'Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), Barcelona, Spain; CIBER de Diabetes y Enfermedades Metabólicas Asociadas (CIBERDEM), Spain.

出版信息

Biochim Biophys Acta. 2013 Nov;1829(11):1175-83. doi: 10.1016/j.bbagrm.2013.08.003. Epub 2013 Aug 9.

DOI:10.1016/j.bbagrm.2013.08.003
PMID:23938248
Abstract

The atonal-related Neurogenin/NeuroD family of basic helix-loop-helix (bHLH) transcription factors comprises potent inducers of neuronal and endocrine differentiation programs in the nervous and digestive system. Atonal homolog 8 (Atoh8) displays high similarity in the bHLH domain with NeuroD proteins. Yet, available evidences indicate that Atoh8 has distinctive features including a ubiquitous expression pattern in embryonic tissues and the ability to inhibit differentiation. To gain insights into Atoh8 function, we aimed at identifying Atoh8 targets and investigated the effects of Atoh8 on global gene expression patterns in pancreatic mPAC cells, a model of bHLH-dependent endocrine differentiation. Our data reveal that Atoh8 is a weak transcriptional activator and does not exhibit proendocrine activity. Conversely, it blocks the induction of a reduced group of gene targets of the atonal-related proendocrine factor Neurogenin3. We show that Atoh8 lacks a transactivation domain and possesses intrinsic repressor activity that depends on a conserved Proline-rich domain. Atoh8 binds the ubiquitous E protein E47 and its ability to repress transcription may partly result from its ability to inhibit E47/E47 and Neurogenin3/E47 dimer activities. These results reveal distinctive transcriptional properties of Atoh8 within the atonal-related bHLH family that may be associated with the acquisition of new biological functions.

摘要

与无调性相关的神经生成素/NeuroD碱性螺旋-环-螺旋(bHLH)转录因子家族是神经和消化系统中神经元及内分泌分化程序的有效诱导因子。无调性同源物8(Atoh8)在bHLH结构域与NeuroD蛋白具有高度相似性。然而,现有证据表明Atoh8具有独特特征,包括在胚胎组织中广泛的表达模式以及抑制分化的能力。为深入了解Atoh8的功能,我们旨在鉴定Atoh8的靶标,并研究Atoh8对胰腺mPAC细胞(一种bHLH依赖性内分泌分化模型)整体基因表达模式的影响。我们的数据显示,Atoh8是一种弱转录激活因子,不表现出促内分泌活性。相反,它会阻断无调性相关促内分泌因子神经生成素3的一组减少的基因靶标的诱导。我们发现Atoh8缺乏反式激活结构域,并具有依赖于保守的富含脯氨酸结构域的内在抑制活性。Atoh8与广泛存在的E蛋白E47结合,其抑制转录的能力可能部分源于其抑制E47/E47和神经生成素3/E47二聚体活性的能力。这些结果揭示了Atoh8在与无调性相关的bHLH家族中的独特转录特性,这可能与新生物学功能的获得有关。

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