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Synthetic beta-solenoid proteins with the fragment-free computational design of a beta-hairpin extension

机译:合成的β-电磁蛋白具有β-发夹延伸的无片段计算设计

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摘要

The ability to design and construct structures with atomic level precision is one of the key goals of nanotechnology. Proteins offer an attractive target for atomic design because they can be synthesized chemically or biologically and can self-assemble. However, the generalized protein folding and design problem is unsolved. One approach to simplifying the problem is to use a repetitive protein as a scaffold. Repeat proteins are intrinsically modular, and their folding and structures are better understood than large globular domains. Here, we have developed a class of synthetic repeat proteins based on the pentapeptide repeat family of beta-solenoid proteins. We have constructed length variants of the basic scaffold and computationally designed de novo loops projecting from the scaffold core. The experimentally solved 3.56-Å resolution crystal structure of one designed loop matches closely the designed hairpin structure, showing the computational design of a backbone extension onto a synthetic protein core without the use of backbone fragments from known structures. Two other loop designs were not clearly resolved in the crystal structures, and one loop appeared to be in an incorrect conformation. We have also shown that the repeat unit can accommodate whole-domain insertions by inserting a domain into one of the designed loops.
机译:具有原子级精度的设计和构造结构的能力是纳米技术的主要目标之一。蛋白质为原子设计提供了一个有吸引力的目标,因为它们可以化学或生物合成并且可以自组装。但是,普遍的蛋白质折叠和设计问题尚未解决。简化问题的一种方法是使用重复蛋白作为支架。重复蛋白本质上是模块化的,其折叠和结构比大球形结构域更好地理解。在这里,我们基于β-电磁蛋白的五肽重复序列家族开发出了一类合成重复序列蛋白。我们构建了基本脚手架的长度变体,并从脚手架核心投射了经过计算设计的de novo循环。通过实验解决的一个设计的环的3.56-Å分辨率晶体结构与设计的发夹结构紧密匹配,显示了在不使用已知结构的骨架片段的情况下,骨架延伸到合成蛋白核上的计算设计。在晶体结构中没有清楚地分辨出另外两个环设计,并且一个环似乎是不正确的构象。我们还表明,通过将一个域插入设计的循环之一中,重复单元可以适应整个域的插入。

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