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Construction of novel repeat proteins with rigid and predictable structures using a shared helix method

机译:使用共享螺旋方法构建具有刚性和可预测结构的新型重复蛋白

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摘要

Generating artificial protein assemblies with complex shapes requires a method for connecting protein components with stable and predictable structures. Currently available methods for creating rigid protein assemblies rely on either complicated calculations or extensive trial and error. We describe a simple and efficient method for connecting two proteins via a fused alpha helix that is formed by joining two preexisting helices into a single extended helix. Because the end-to-end ligation of helices does not guarantee the formation of a continuous helix, we superimposed 1–2 turns of pairs of connecting helices by using a molecular graphics program. Then, we chose amino acids from the two natural sequences that would stabilize the connecting helix. This “shared helix method” is highly efficient. All the designed proteins that could be produced in Escherichia coli were readily crystallized and had the expected fusion structures. To prove the usefulness of this method, we produced two novel repeat proteins by assembling several copies of natural or artificial proteins with alpha helices at both termini. Their crystal structures demonstrated the successful assembly of the repeating units with the intended curved shapes. We propose that this method could dramatically expand the available repertoire of natural repeat proteins.
机译:生成具有复杂形状的人造蛋白质装配体需要一种将蛋白质成分与稳定且可预测的结构相连接的方法。创建刚性蛋白质装配体的当前可用方法依赖于复杂的计算或大量的反复试验。我们描述了一种简单有效的方法,用于通过将两个预先存在的螺旋连接成一个单独的延伸螺旋而形成的融合α螺旋来连接两个蛋白质。由于螺旋的端对端连接不能保证形成连续的螺旋,因此我们使用分子图形程序将1-2对成对的连接螺旋叠加在一起。然后,我们从两个可以稳定连接螺旋的天然序列中选择氨基酸。这种“共享螺旋法”非常有效。可以在大肠杆菌中生产的所有设计蛋白都容易结晶,并具有预期的融合结构。为了证明该方法的有效性,我们通过在两个末端均带有α螺旋的天然或人工蛋白质的多个拷贝进行组装,产生了两个新颖的重复蛋白质。他们的晶体结构证明了具有预期弯曲形状的重复单元的成功组装。我们建议这种方法可以大大扩展自然重复蛋白的可用库。

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