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Role of the maize transcription factor R in the regulation of anthocyanin biosynthesis.

机译:玉米转录因子R在花色苷生物合成调控中的作用。

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摘要

The maize flavonoid biosynthetic pathway is one of the best characterized plant model systems to study the combinatorial regulation of gene expression. Flavonoids are important secondary metabolites and important for the plant, such as in the case for anthocyanins as attractants to pollinators as well as for humans due to a number of biological activities. Anthocyanins in maize are regulated by the cooperation of the R2R3-MYB domain protein C1 and the basic helix-loop-helix (bHLH) protein R. In contrast, phlobaphene pigments, derived from a separate flavonoid biosynthetic branch, are regulated by the R2R3-MYB domain protein P1, which can activate transcription in the absence of a (known) bHLH. Our laboratory has established that the bHLH transcription factor R plays a key role in determining the biological specificity of C1. I describe here how R might contribute to regulatory specificity, on one hand by forming a platform for protein-protein interactions, and on another, by binding to different sites in the regulatory regions of its target genes depending on the interacting partners. Using a variety of techniques I have investigated three protein-protein interacting regions of R. I demonstrate that the highly conserved bHLH domain of R is involved in transcriptional regulation and histone functions. I show that R interacts with the EMSY-like protein RIF1 specifically via the bHLH domain and that this interaction is required for the regulation of endogenous flavonoid genes. RIF1 is part of the C1/R regulatory complex and I discuss how RIF1 links transcriptional regulation of flavonoid biosynthetic genes with chromatin function. In addition, I show that the region adjacent to the bHLH domain has structural similarity to a leucine zipper and that the extended bHLH-LZ-like region is able to homodimerize. The bHLH-LZ-like mediated dimerization is required for activation of a synthetic pG-box::Luc promoter::reporter construct in transient expression studies and for binding to a synthetic G-box probe, as well as to the Bz1 and C2 promoter in vitro. Furthermore, I demonstrate that the ACT domain at the C-terminus of R homodimerizes. This domain is necessary for anthocyanin pigment formation, for transcriptional activation of at least four anthocyanin biosynthetic genes and important for DNA-binding to the A1 and Bz1 promoters. I show that interplay between the functional domains described here is necessary for transcriptional activation and DNA-binding. I am also characterizing R-interacting partners which possibly tether R to as yet unknown target genes and therefore might show the involvement of R in other cellular processes.;Taken together, these studies emphasize the importance of the bHLH transcription factor R in combinatorial regulation of gene expression of anthocyanin biosynthetic genes and open new possibilities for R to function in other cellular processes. Moreover, these studies highlight the complexity of biochemical pathway regulation and show novel mechanisms of how one TF can participate in several regulatory complexes.
机译:玉米黄酮生物合成途径是研究基因表达的组合调控的特征最强的植物模型系统之一。类黄酮是重要的次生代谢产物,对植物也很重要,例如由于许多生物活性,花色苷作为传粉媒介的诱剂以及人类。玉米中的花色苷受R2R3-MYB结构域蛋白C1和基本螺旋-环-螺旋(bHLH)蛋白R的共同调控。相比之下,来源于单独的类黄酮生物合成分支的酞菁色素则受R2R3-调控。 MYB域蛋白P1,可以在不存在(已知)bHLH的情况下激活转录。我们的实验室已经确定,bHLH转录因子R在确定C1的生物学特异性中起关键作用。我在这里描述R如何一方面通过形成蛋白质-蛋白质相互作用的平台,另一方面通过结合其靶基因调节区域中取决于相互作用伙伴的不同位点而对调节特异性作出贡献。我使用多种技术研究了R的三个蛋白质-蛋白质相互作用区域。我证明R的高度保守的bHLH结构域参与转录调节和组蛋白功能。我表明R特别通过bHLH域与EMSY样蛋白RIF1相互作用,并且这种相互作用是调节内源性类黄酮基因所必需的。 RIF1是C1 / R调节复合物的一部分,我将讨论RIF1如何将类黄酮生物合成基因的转录调节与染色质功能联系起来。另外,我显示了与bHLH结构域相邻的区域与亮氨酸拉链具有结构相似性,并且扩展的bHLH-LZ样区域能够均二聚化。在瞬时表达研究中激活合成pG-box :: Luc启动子:: reporter构建体以及与合成G-box探针以及Bz1和C2启动子结合均需要bHLH-LZ样介导的二聚化作用体外。此外,我证明了在R的C末端的ACT域同源二聚体。该结构域对于花色苷色素的形成,至少四个花色苷生物合成基因的转录激活是必需的,并且对于DNA与A1和Bz1启动子的结合至关重要。我表明,此处描述的功能域之间的相互作用对于转录激活和DNA结合是必需的。我还表征了R相互作用的伙伴,这些伙伴可能将R束缚到未知的靶基因上,因此可能表明R参与了其他细胞过程。总而言之,这些研究强调了bHLH转录因子R在对HHL的组合调控中的重要性。花青素生物合成基因的基因表达,并为R在其他细胞过程中发挥功能开辟了新的可能性。此外,这些研究突出了生化途径调控的复杂性,并显示了一种TF如何参与多种调控复合物的新颖机制。

著录项

  • 作者

    Feller, Antje Christin.;

  • 作者单位

    The Ohio State University.;

  • 授予单位 The Ohio State University.;
  • 学科 Biology Molecular.
  • 学位 Ph.D.
  • 年度 2010
  • 页码 207 p.
  • 总页数 207
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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