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首页> 外文期刊>Chembiochem: A European journal of chemical biology >Site-Specific Isotopic Labeling (SSIL): Access to High-Resolution Structural and Dynamic Information in Low-Complexity Proteins
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Site-Specific Isotopic Labeling (SSIL): Access to High-Resolution Structural and Dynamic Information in Low-Complexity Proteins

机译:特异性同位素标记(SSIL):获得低复杂性蛋白质中的高分辨率结构和动态信息

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摘要

Remarkable technical progress in the area of structural biology has paved the way to study previously inaccessible targets. For example, large protein complexes can now be easily investigated by cryo-electron microscopy, and modern high-field NMR magnets have challenged the limits of high-resolution characterization of proteins in solution. However, the structural and dynamic characteristics of certain proteins with important functions still cannot be probed by conventional methods. These proteins in question contain low-complexity regions (LCRs), compositionally biased sequences where only a limited number of amino acids is repeated multiple times, which hamper their characterization. This Concept article describes a site-specific isotopic labeling (SSIL) strategy, which combines nonsense suppression and cell-free protein synthesis to overcome these limitations. An overview on how poly-glutamine tracts were made amenable to high-resolution structural studies is used to illustrate the usefulness of SSIL. Furthermore, we discuss the potential of this methodology to give further insights into the roles of LCRs in human pathologies and liquid-liquid phase separation, as well as the challenges that must be addressed in the future for the popularization of SSIL.
机译:结构生物学领域的显着技术进步已经为先前无法访问的目标铺平了途径。例如,现在可以通过冷冻电子显微镜容易地研究大的蛋白质复合物,并且现代高场NMR磁体挑战溶液中蛋白质的高分辨率表征的限制。然而,通过常规方法仍然无法探测具有重要功能的某些蛋白质的结构和动态特性。有问题的这些蛋白质含有低复杂性区域(LCRS),其中仅多次重复有限数量的氨基酸的合成偏置序列,其妨碍其表征。这篇概念文章介绍了一种特异性特异性同位素标记(SSIL)策略,其结合了非阵容抑制和无细胞蛋白质合成来克服这些限制。概述了多谷氨酰胺在高分辨率结构研究方面是如何进行的,用于说明SSIL的有用性。此外,我们讨论了这种方法的潜力,以进一步了解LCRS在人类病理和液体相分离中的作用,以及在未来必须在SSIL的普及中解决的挑战。

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