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通过调控转录因子相互作用进行信号传导:Myb相关蛋白Bas1p中调控相互作用结构域的定位

Signaling through regulated transcription factor interaction: mapping of a regulatory interaction domain in the Myb-related Bas1p.

作者信息

Pinson B, Kongsrud T L, Ording E, Johansen L, Daignan-Fornier B, Gabrielsen O S

机构信息

Department of Biochemistry, University of Oslo, PO Box 1041, Blindern, N-0316 Oslo 3, Norway.

出版信息

Nucleic Acids Res. 2000 Dec 1;28(23):4665-73. doi: 10.1093/nar/28.23.4665.

Abstract

Gene activation in eukaryotes is inherently combinatorial depending on cooperation between different transcription factors. An example where this cooperation seems to be directly exploited for regulation is the Bas1p/Bas2p couple in yeast. Bas1p is a Myb-related transcription factor that acts together with the homeodomain-related Bas2p (Pho2p) to regulate purine and histidine biosynthesis genes in response to extracellular purine limitation. We show that fusion of the two factors abolished adenine repression, suggesting that what is regulated by adenine is the Bas1p-Bas2p interaction. Analysis of Bas1p deletions revealed a critical domain (Bas1p interaction and regulatory domain, BIRD) acting in two-hybrid assays as an adenine-dependent Bas1p-Bas2p interaction domain. BIRD had a dual function, as an internal repressor of a centrally located Bas1p transactivation domain on the ADE1 promoter and as a Bas2p-dependent activator on the HIS4 promoter. This promoter-dependent behavior reflected a differential binding to the two promoters in vivo. On ADE1 Bas1p bound the promoter efficiently by itself, but required adenine limitation and Bas2p interaction through BIRD for derepression. On HIS4 efficient promoter binding and derepression required both factors and adenine limitation. We propose a promoter-dependent model for adenine regulation in yeast based on controlled Bas1p-Bas2p interactions through BIRD and exploited differentially by the two promoters.

摘要

真核生物中的基因激活本质上是组合式的,这取决于不同转录因子之间的协同作用。酵母中的Bas1p/Bas2p组合似乎是直接利用这种协同作用进行调控的一个例子。Bas1p是一种与Myb相关的转录因子,它与同源结构域相关的Bas2p(Pho2p)共同作用,以响应细胞外嘌呤限制来调节嘌呤和组氨酸生物合成基因。我们发现,将这两种因子融合会消除腺嘌呤抑制作用,这表明腺嘌呤所调控的是Bas1p-Bas2p相互作用。对Bas1p缺失的分析揭示了一个关键结构域(Bas1p相互作用和调节结构域,BIRD),在双杂交实验中它作为一个依赖腺嘌呤的Bas1p-Bas2p相互作用结构域发挥作用。BIRD具有双重功能,作为ADE1启动子上位于中心位置的Bas1p反式激活结构域的内部抑制因子,以及作为HIS4启动子上依赖Bas2p的激活因子。这种启动子依赖性行为反映了在体内与两个启动子的不同结合情况。在ADE1上,Bas1p自身能有效结合启动子,但需要腺嘌呤限制以及通过BIRD与Bas2p相互作用才能解除抑制。在HIS4上,有效的启动子结合和解除抑制需要这两种因子以及腺嘌呤限制。我们基于通过BIRD控制的Bas1p-Bas2p相互作用,并由两个启动子进行不同利用,提出了酵母中腺嘌呤调控的启动子依赖性模型。

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