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重叠的激活因子和抑制因子界定了果蝇眼中对受体酪氨酸激酶信号的转录反应。

Overlapping activators and repressors delimit transcriptional response to receptor tyrosine kinase signals in the Drosophila eye.

作者信息

Xu C, Kauffmann R C, Zhang J, Kladny S, Carthew R W

机构信息

Department of Biological Sciences, University of Pittsburgh, Pennsylvania 15260, USA.

出版信息

Cell. 2000 Sep 29;103(1):87-97. doi: 10.1016/s0092-8674(00)00107-0.

Abstract

Regulated transcription of the prospero gene in the Drosophila eye provides a model for how gene expression is specifically controlled by signals from receptor tyrosine kinases. We show that prospero is controlled by signals from the EGF receptor DER and the Sevenless receptor. A direct link is established between DER activation of a transcription enhancer in prospero and binding of two transcription factors that are targets of DER signaling. Binding of the cell-specific Lozenge protein is also required for activation, and overlapping Lozenge protein distribution and DER signaling establishes expression in a subset of equivalent cells competent to respond to Sevenless. We show that Sevenless activates prospero independent of the enhancer and involves targeted degradation of Tramtrack, a transcription repressor.

摘要

果蝇眼中prospero基因的转录调控为基因表达如何由受体酪氨酸激酶发出的信号特异性控制提供了一个模型。我们发现prospero受表皮生长因子受体DER和Sevenless受体发出的信号控制。prospero中转录增强子的DER激活与作为DER信号传导靶点的两个转录因子的结合之间建立了直接联系。细胞特异性的菱形蛋白的结合对于激活也是必需的,并且菱形蛋白分布与DER信号传导的重叠在一组有能力响应Sevenless的等效细胞的子集中建立了表达。我们发现Sevenless独立于增强子激活prospero,并且涉及转录抑制因子Tramtrack的靶向降解。

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