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(βα)-桶状蛋白中的重复序列结构基序和基于此类基序设计的嵌合蛋白的实验优化。

Recurring sequence-structure motifs in (βα)-barrel proteins and experimental optimization of a chimeric protein designed based on such motifs.

机构信息

School of Life Sciences, University of Science and Technology of China, Hefei, Anhui 230027, China.

School of Life Sciences, University of Science and Technology of China, Hefei, Anhui 230027, China; Hefei National Laboratory for Physical Sciences at the Microscale, Hefei, Anhui 230027, China; Hefei Institutes of Physical Science, Chinese Academy of Sciences, Hefei, Anhui 230031, China.

出版信息

Biochim Biophys Acta Proteins Proteom. 2017 Feb;1865(2):165-175. doi: 10.1016/j.bbapap.2016.11.001. Epub 2016 Nov 9.

Abstract

An interesting way of generating novel artificial proteins is to combine sequence motifs from natural proteins, mimicking the evolutionary path suggested by natural proteins comprising recurring motifs. We analyzed the βα and αβ modules of TIM barrel proteins by structure alignment-based sequence clustering. A number of preferred motifs were identified. A chimeric TIM was designed by using recurring elements as mutually compatible interfaces. The foldability of the designed TIM protein was then significantly improved by six rounds of directed evolution. The melting temperature has been improved by more than 20°C. A variety of characteristics suggested that the resulting protein is well-folded. Our analysis provided a library of peptide motifs that is potentially useful for different protein engineering studies. The protein engineering strategy of using recurring motifs as interfaces to connect partial natural proteins may be applied to other protein folds.

摘要

生成新型人工蛋白质的一种有趣方法是组合天然蛋白质的序列基序,模拟由包含重复基序的天然蛋白质所暗示的进化路径。我们通过基于结构比对的序列聚类分析 TIM 桶蛋白的βα和αβ模块。确定了一些优选的基序。通过使用重复元件作为相互兼容的界面,设计了一种嵌合 TIM。通过六轮定向进化,显著提高了设计的 TIM 蛋白的折叠能力。熔点提高了 20°C 以上。多种特性表明,所得蛋白质折叠良好。我们的分析提供了一个潜在可用于各种蛋白质工程研究的肽基序文库。使用重复基序作为界面连接部分天然蛋白质的蛋白质工程策略可应用于其他蛋白质折叠。

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