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同源结构域蛋白对核信号转导通路的序列特异性靶向作用。

Sequence-specific targeting of nuclear signal transduction pathways by homeodomain proteins.

作者信息

Grueneberg D A, Simon K J, Brennan K, Gilman M

机构信息

Cold Spring Harbor Laboratory, New York 11724, USA.

出版信息

Mol Cell Biol. 1995 Jun;15(6):3318-26. doi: 10.1128/MCB.15.6.3318.

DOI:10.1128/MCB.15.6.3318
PMID:7760827
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC230565/
Abstract

Cells translate extracellular signals into specific programs of gene expression that reflect their developmental history or identity. We present evidence that one way this interpretation may be performed is by cooperative interactions between serum response factor (SRF) and certain homeodomain proteins. We show that human and Drosophila homeodomain proteins of the paired class have the ability to recruit SRF to DNA sequences not efficiently recognized by SRF on its own, thereby imparting to a linked reporter gene the potential to respond to polypeptide growth factors. This activity requires both the DNA-binding activity of the homeodomain and putative protein-protein contact residues on the exposed surfaces of homeodomain helices 1 and 2. The ability of the homeodomain to impart signal responsiveness is DNA sequence specific, and this specificity differs from the simple DNA-binding specificity of the homeodomain in vitro. The homeodomain imparts response to a spectrum of signals characteristic of the natural SRF-binding site in the c-fos gene. Response to some of these signals is dependent on the secondary recruitment of SRF-dependent ternary complex factors, and we show directly that a homeodomain can promote the recruitment of one such factor, Elk1. We infer that SRF and homeodomains interact cooperatively on DNA and that formation of SRF-homeodomain complexes permits the recruitment of signal-responsive SRF accessory proteins. The ability to route extracellular signals to specific target genes is a novel activity of the homeodomain, which may contribute to the identity function displayed by many homeodomain genes.

摘要

细胞将细胞外信号转化为反映其发育历史或身份的特定基因表达程序。我们提供的证据表明,这种解读可能通过血清反应因子(SRF)与某些同源结构域蛋白之间的协同相互作用来实现。我们发现,配对类别的人类和果蝇同源结构域蛋白能够将SRF招募到其自身无法有效识别的DNA序列上,从而赋予相连的报告基因对多肽生长因子作出反应的潜力。这种活性既需要同源结构域的DNA结合活性,也需要同源结构域螺旋1和2暴露表面上假定的蛋白质-蛋白质接触残基。同源结构域赋予信号反应性的能力是DNA序列特异性的,且这种特异性不同于同源结构域在体外的简单DNA结合特异性。同源结构域赋予对c-fos基因中天然SRF结合位点特有的一系列信号的反应性。对其中一些信号的反应依赖于SRF依赖性三元复合因子的二次招募,并且我们直接表明同源结构域可以促进招募其中一种因子Elk1。我们推断,SRF和同源结构域在DNA上协同相互作用,并且SRF-同源结构域复合物的形成允许招募信号反应性SRF辅助蛋白。将细胞外信号导向特定靶基因的能力是同源结构域的一种新活性,这可能有助于许多同源结构域基因所发挥的身份功能。

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