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首页> 外文期刊>Nucleic Acids Research >Multiple receptor interaction domains of GRIP1 function in synergy.
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Multiple receptor interaction domains of GRIP1 function in synergy.

机译:GRIP1的多个受体相互作用域发挥协同作用。

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Nuclear hormone receptors are exerting their effect on transcription by interacting with basal factors of the transcription machinery and/or by recruiting intermediary factors, such as the mouse protein GRIP1. GRIP1 is one of the recently identified coactivators for nuclear hormone receptors. Upon interaction with the hormone-binding domain of the receptors, GRIP1 increases their transcriptional activity. Here we show that GRIP1 contains at least two receptor-interacting regions using the hormone-binding domain of several receptors as bait in the yeast two-hybrid assay. GRIP1 interacts in a hormone-dependent manner with the C-termini of nuclear hormone receptors such as GRalpha, TRalpha, TRbeta, RARalpha and RXRalpha but not with v-ErbA. GRIP1 contains several LXXLL motifs which were shown to be required for receptor interaction. A protein fragment containing all of the three LXXLL motifs, but having the activation domain deleted, is able to repress the transcriptional activity of human TRbeta, whereas a region harbouring only one LXXLL motif fails to do so. A protein fragment with two LXXLL motifs exhibits an intermediate modulation of the TRbeta transactivation. While one motif seems to be sufficient for receptor interaction, more than one motif is needed for functional interference.
机译:核激素受体通过与转录机制的基础因子相互作用和/或通过募集中介因子(例如小鼠蛋白GRIP1),对转录发挥作用。 GRIP1是最近确定的核激素受体共激活剂之一。与受体的激素结合域相互作用后,GRIP1会增加其转录活性。在这里,我们显示了GRIP1包含至少两个受体相互作用区域,使用几种受体的激素结合结构域作为酵母双杂交检测中的诱饵。 GRIP1以激素依赖性方式与核激素受体(例如GRalpha,TRalpha,TRbeta,RARalpha和RXRalpha)的C末端相互作用,但不与v-ErbA相互作用。 GRIP1包含几个LXXLL基序,这些基序被证明是受体相互作用所必需的。包含所有三个LXXLL基序但缺失了激活结构域的蛋白质片段能够抑制人TRbeta的转录活性,而仅包含一个LXXLL基序的区域则不能。具有两个LXXLL基序的蛋白质片段表现出TRbeta反式激活的中间调节。尽管一个基序似乎足以实现受体相互作用,但功能干扰需要一个以上的基序。

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