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原神经碱性螺旋-环-螺旋转录因子的螺旋-环-螺旋结构域决定了下游靶标激活的不同模式。

Distinct patterns of downstream target activation are specified by the helix-loop-helix domain of proneural basic helix-loop-helix transcription factors.

作者信息

Talikka Marja, Perez Sharon E, Zimmerman Kathryn

机构信息

Laboratory of Developmental Neurobiology, The Rockefeller University, 1230 York Avenue, New York, New York 10021, USA.

出版信息

Dev Biol. 2002 Jul 1;247(1):137-48. doi: 10.1006/dbio.2002.0677.

Abstract

Both gain- and loss-of-function analyses indicate that proneural basic/helix-loop-helix (bHLH) proteins direct not only general aspects of neuronal differentiation but also specific aspects of neuronal identity within neural progenitors. In order to better understand the function of this family of transcription factors, we have used hormone-inducible fusion constructs to assay temporal patterns of downstream target regulation in response to proneural bHLH overexpression. In these studies, we have compared two distantly related Xenopus proneural bHLH genes, Xash1 and XNgnr1. Our findings indicate that both Xash1 and XNgnr1 induce expression of the general neuronal differentiation marker, N-tubulin, with a similar time course in animal cap progenitor populations. In contrast, these genes each induce distinct patterns of early downstream target expression. Both genes induce expression of the HLH-containing gene, Xcoe2, at early time points, but only XNgnr1 induces early expression of the bHLH genes, Xath3 and XNeuroD. Structure:function analyses indicate that the distinct pattern of XNgnr1-induced downstream target activation is linked to the XNgnr1 HLH domain, demonstrating a novel role for this domain in mediating the differential function of individual members of the proneural bHLH gene family.

摘要

功能获得和功能丧失分析均表明,原神经碱性/螺旋-环-螺旋(bHLH)蛋白不仅指导神经元分化的一般方面,还指导神经祖细胞内神经元身份的特定方面。为了更好地理解这个转录因子家族的功能,我们使用了激素诱导融合构建体来检测响应原神经bHLH过表达时下游靶标调控的时间模式。在这些研究中,我们比较了两个远缘相关的非洲爪蟾原神经bHLH基因,Xash1和XNgnr1。我们的研究结果表明,Xash1和XNgnr1在动物帽祖细胞群体中以相似的时间进程诱导一般神经元分化标志物N-微管蛋白的表达。相比之下,这些基因各自诱导不同的早期下游靶标表达模式。两个基因在早期时间点均诱导含HLH的基因Xcoe2的表达,但只有XNgnr1诱导bHLH基因Xath3和XNeuroD的早期表达。结构-功能分析表明,XNgnr1诱导的下游靶标激活的独特模式与XNgnr1的HLH结构域相关,证明了该结构域在介导原神经bHLH基因家族单个成员的差异功能中的新作用。

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