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首页> 外文期刊>Seminars in cancer biology >Structural determinants of 14-3-3 binding specificities and regulation of subcellular localization of 14-3-3-ligand complexes: a comparison of the X-ray crystal structures of all human 14-3-3 isoforms.
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Structural determinants of 14-3-3 binding specificities and regulation of subcellular localization of 14-3-3-ligand complexes: a comparison of the X-ray crystal structures of all human 14-3-3 isoforms.

机译:14-3-3结合特异性的结构决定因素和14-3-3-配体复合物的亚细胞定位调控:所有人类14-3-3同工型的X射线晶体结构比较。

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摘要

14-3-3 proteins are a ubiquitous class of regulatory proteins found in all eukaryotic cells and were the first class of molecules to be recognized as discrete phosphoserine/threonine binding modules. 14-3-3 proteins bind a large number of different substrates to regulate a wide array of cellular signaling events including cell cycle progression and DNA damage responses, programmed cell death, cytoskeletal dynamics, transcriptional control of gene expression, as well as processes directly related to cancer progression. In this review, the structural basis of phosphorylation-dependent binding of 14-3-3 to peptide and protein ligands is discussed along with mechanisms that govern how 14-3-3 regulates the function of its bound ligands. The X-ray crystal structures of all human 14-3-3 proteins bound to peptides have now been solved. Here, we use structural comparisons between isoforms as a framework for discussion of ligand binding by 14-3-3 as well as the mechanisms through which post-translational modification of the different isoforms alters their function.
机译:14-3-3蛋白是在所有真核细胞中普遍存在的一类调节蛋白,并且是被识别为离散的磷酸丝氨酸/苏氨酸结合模块的第一类分子。 14-3-3蛋白与大量不同的底物结合以调节多种细胞信号转导事件,包括细胞周期进程和DNA损伤反应,程序性细胞死亡,细胞骨架动力学,基因表达的转录控制以及直接相关的过程癌症进展。在这篇综述中,讨论了14-3-3与肽和蛋白质配体的磷酸化依赖性结合的结构基础,以及控制14-3-3如何调节其结合配体功能的机制。现在已经解决了与肽结合的所有人类14-3-3蛋白的X射线晶体结构。在这里,我们使用同工型之间的结构比较作为讨论14-3-3配体结合的框架,以及不同同工型的翻译后修饰改变其功能的机制。

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