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Single-molecule FRET and crosslinking studies in structural biology enabled by noncanonical amino acids

机译:非规范氨基酸在结构生物学中的单分子FRET和交联研究

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Contemporary structural biology research promises more than just static snap-shots of molecular machineries. This goal is not just facilitated by combining different structural biology techniques, but also by new tools from the field of protein and genetic engineering, as well as from chemistry. Genetic encoding of noncanonical amino acids (ncAAs) through codon-suppression technology provides an excellent opportunity to probe biomolecules using different structural biology methods. In this article, we review the applications of ncAA incorporation into proteins for determining structural information through various techniques with the main focus on crosslinking mass spectrometry and single-molecule FRET-based techniques. Furthermore, advances and limitations of the incorporation of multiple ncAAs are discussed, with respect to design of an ideal host organism for modern and integrative structural biology research.
机译:当代结构生物学研究承诺的不仅仅是分子机械的静态快照。不仅可以通过结合不同的结构生物学技术来实现此目标,而且可以通过蛋白质和基因工程领域以及化学领域的新工具来实现。通过密码子抑制技术对非规范氨基酸(ncAAs)进行遗传编码,为使用不同结构生物学方法探查生物分子提供了极好的机会。在本文中,我们回顾了将ncAA掺入蛋白质中以通过各种技术确定结构信息的应用,主要侧重于交联质谱法和基于单分子FRET的技术。此外,就设计用于现代和整合结构生物学研究的理想宿主生物而言,讨论了结合多种ncAA的进展和局限性。

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