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Ubiquitin Interacting Motifs: Duality Between Structured and Disordered Motifs

机译:泛素互动图案:结构化和紊乱的主题之间的二元性

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Ubiquitin is a small protein at the heart of many cellular processes, and several different protein domains are known to recognize and bind ubiquitin. A common motif for interaction with ubiquitin is the Ubiquitin Interacting Motif (UIM), characterized by a conserved sequence signature and often found in multi-domain proteins. Multi-domain proteins with intrinsically disordered regions mediate interactions with multiple partners, orchestrating diverse pathways. Short linear motifs for binding are often embedded in these disordered regions and play crucial roles in modulating protein function. In this work, we investigated the structural propensities of UIMs using molecular dynamics simulations and NMR chemical shifts. Despite the structural portrait depicted by X-crystallography of stable helical structures, we show that UIMs feature for both helical or intrinsically disordered motifs. Our results shed light on a new class of disordered UIMs. This group is here exemplified by the C-terminal domain of one isoform of ataxin-3 and a group of USP-containing proteins. Intriguingly, UIMs not only bind ubiquitin. They can be a recruitment point for other interactors, such as parkin and heat shock protein Hsc70-4. Disordered UIMs can provide versatility and new functions to the client proteins, opening new venues for research on their interactome.
机译:泛素是许多细胞过程中核心的小蛋白质,已知几个不同的蛋白质结构域识别并结合泛素。与泛素相互作用的常见主题是泛素相互作用的基序(UIM),其特征在于保守的序列签名,经常在多域蛋白中发现。具有本质无序区域的多域蛋白介导与多个伴侣的相互作用,协调各种途径。结合的短线性图案通常嵌入在这些无序区域中,并在调节蛋白质功能方面发挥关键作用。在这项工作中,我们调查了使用分子动力学模拟和NMR化学位移的UIM的结构性促使。尽管稳定螺旋结构的X晶片图所描绘的结构画像,但我们表明UIMS为螺旋或本质上无序的图案。我们的结果阐明了一类新的无序UIM。该组在这里由ATAXIN-3的一种同种型的C末端结构域和一组含USP的蛋白质。有趣的,UIM不仅结合泛素。它们可以成为其他互动者的招聘点,例如Parkin和热休克蛋白HSC70-4。无序的UIM可以为客户蛋白提供多功能性和新功能,为其互乱组开设新场地。

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