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首页> 外文期刊>Nucleic acids research >The PXDLS linear motif regulates circadian rhythmicity through protein–protein interactions
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The PXDLS linear motif regulates circadian rhythmicity through protein–protein interactions

机译:PXDLS线性基序通过蛋白质间相互作用调节昼夜节律

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摘要

The circadian core clock circuitry relies on interlocked transcription-translation feedback loops that largely count on multiple protein interactions. The molecular mechanisms implicated in the assembly of these protein complexes are relatively unknown. Our bioinformatics analysis of short linear motifs, implicated in protein interactions, reveals an enrichment of the Pro-X-Asp-Leu-Ser (PXDLS) motif within circadian transcripts. We show that the PXDLS motif can bind to BMAL1/CLOCK and disrupt circadian oscillations in a cell-autonomous manner. Remarkably, the motif is evolutionary conserved in the core clock protein REV-ERBα, and additional proteins implicated in the clock's function (NRIP1, CBP). In this conjuncture, we uncover a novel cross talk between the two principal core clock feedback loops and show that BMAL/CLOCK and REV-ERBα interact and that the PXDLS motif of REV-ERBα participates in their binding. Furthermore, we demonstrate that the PXDLS motifs of NRIP1 and CBP are involved in circadian rhythmicity. Our findings suggest that the PXDLS motif plays an important role in circadian rhythmicity through regulation of protein interactions within the clock circuitry and that short linear motifs can be employed to modulate circadian oscillations.
机译:昼夜节律核心时钟电路依赖于互锁的转录-翻译反馈回路,该回路主要依靠多种蛋白质相互作用。这些蛋白质复合物的组装涉及的分子机制是相对未知的。我们对涉及蛋白质相互作用的短线性基序的生物信息学分析揭示了昼夜节律转录本中Pro-X-Asp-Leu-Ser(PXDLS)基序的富集。我们表明,PXDLS母题可以绑定到BMAL1 / CLOCK,并以细胞自主方式破坏昼夜节律振荡。值得注意的是,该基序在核心时钟蛋白REV-ERBα中是进化保守的,而在时钟功能中还涉及其他蛋白(NRIP1,CBP)。在这个关键时刻,我们发现了两个主要核心时钟反馈回路之间的新颖串扰,并表明BMAL / CLOCK和REV-ERBα相互作用,并且REV-ERBα的PXDLS基序参与其结合。此外,我们证明了NRIP1和CBP的PXDLS主题参与了昼夜节律。我们的发现表明,PXDLS基序通过调节时钟电路内的蛋白质相互作用在昼夜节律中起重要作用,而短的线性基序可用于调节昼夜节律。

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