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Intersubunit linker length as a modifier of protein stability: Crystal structures and thermostability of mutant TRAP

机译:亚基间连接子长度作为蛋白质稳定性的调节剂:突变TRAP的晶体结构和热稳定性

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摘要

The ability of proteins to self-assemble into complex, functional nanoscale structures is expected to become of significant use in the manufacture of artificial nanodevices with a wide range of novel applications. The bacterial protein TRAP has potential uses as a nanoscale component as it is ring-shaped, with a central, modifiable cavity. Furthermore, it can be engineered to make a ring of 12-fold symmetry, which is advantageous for packing into two-dimensional arrays. The 12mer form of TRAP is made by linking multiple subunits together on the same polypeptide, but the usefulness of the 12mers described to date is limited by their poor stability. Here we show that, by altering the length of the peptide linker between subunits, the thermostability can be significantly improved. Since the subunit interfaces of the different 12mers are essentially identical, stabilization arises from the reduction of strain in the linkers. Such a simple method of controlling the stability of modular proteins may have wide applications, and demonstrates the lack of absolute correlation between interactions observable by crystallography and the internal energy of a complex.
机译:预期蛋白质自组装为复杂的功能性纳米级结构的能力将在具有广泛的新颖应用的人造纳米装置的制造中具有重要用途。细菌蛋白TRAP具有环形,中央可修饰腔体,因此具有作为纳米级成分的潜在用途。此外,可以将其设计成制成12倍对称的环,这对于包装成二维阵列是有利的。 TRAP的12聚体形式是通过将同一多肽上的多个亚基连接在一起而制得的,但迄今为止描述的12聚体的实用性由于其较差的稳定性而受到限制。在这里我们表明,通过改变亚基之间的肽接头的长度,可以显着提高热稳定性。由于不同的12聚体的亚基界面基本上是相同的,因此通过减少接头中的应变可产生稳定作用。这种控制模块蛋白稳定性的简单方法可能具有广泛的应用,并且证明了通过晶体学可观察到的相互作用与复合物的内部能量之间缺乏绝对的相关性。

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