首页> 外文期刊>The Plant Cell >SHORT HYPOCOTYL UNDER BLUE1 Truncations and Mutations Alter Its Association with a Signaling Protein Complex in Arabidopsis.
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SHORT HYPOCOTYL UNDER BLUE1 Truncations and Mutations Alter Its Association with a Signaling Protein Complex in Arabidopsis.

机译:BLUE1下的短朴素截短和突变改变了它与拟南芥中信号蛋白复合物的联系。

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Higher plants monitor their ambient light signals through red/far-red absorbing phytochromes and blue/UV-A light absorbing cryptochromes. Subsequent signaling cascades alter gene expression and initiate morphogenic responses. We previously isolated SHORT HYPOCOTYL UNDER BLUE1 (SHB1), a putative transcriptional coactivator in light signaling. SHB1 is homologous to the SYG1 protein family and contains an N-terminal SPX domain and a C-terminal EXS domain. Overaccumulation of the SPX domain caused a long hypocotyl phenotype similar to that of shb1-D under red, far-red, or blue light. By contrast, overaccumulation of the C-terminal EXS domain led to a short hypocotyl phenotype similar to that of shb1 under blue light. The N-terminal SPX domain was associated with a smaller protein complex than the native protein complex associated with endogenous SHB1. By contrast, the EXS domain was associated with a slightly smaller protein complex than the native protein complex, but it largely displaced endogenous SHB1 from its native protein complex. In addition, all six missense mutations that we identified from a suppressor screen were clustered within or close to the SPX domain, and these mutations impaired the assembly of the SHB1-containing protein complex. We propose that both SPX and EXS domains likely anchor SHB1 to a protein complex, and the SPX domain is critical for SHB1 signaling.
机译:高等植物通过吸收红色/远红色的植物色素和吸收蓝色/ UV-A的隐色染料监视环境光信号。随后的信号级联改变基因表达并启动形态发生反应。我们先前分离了在BLUE1(SHB1)下的短质油素,SHB1是光信号中的一种假定的转录共激活因子。 SHB1与SYG1蛋白家族同源,并包含一个N末端SPX域和一个C末端EXS域。在红色,远红色或蓝色光下,SPX域的过度积累会导致类似于shb1-D的长下胚轴表型。相比之下,C端EXS结构域的过度积累导致了类似于shb1在蓝光下的短下胚轴表型。 N末端SPX域与比与内源性SHB1相关的天然蛋白质复合物更小的蛋白质复合物相关。相比之下,EXS结构域与蛋白质复合物的关系要比天然蛋白质复合物小,但它大大取代了天然蛋白质复合物中的内源性SHB1。此外,我们从抑制子筛选中发现的所有六个错义突变都聚集在SPX域内或附近,并且这些突变削弱了含SHB1蛋白复合体的组装。我们建议SPX和EXS域都可能将SHB1锚定到蛋白质复合物,并且SPX域对于SHB1信号传导至关重要。

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