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Molecular recognition of ubiquitin and Lys63-linked diubiquitin by STAM2 UIM-SH3 dual domain: the effect of its linker length and flexibility

机译:STAM2 UIM-SH3双结构域对泛素和与Lys63连接的双泛素的分子识别:其接头长度和柔性的影响

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摘要

Multidomain proteins represent a broad spectrum of the protein landscape and are involved in various interactions. They could be considered as modular building blocks assembled in distinct fashion and connected by linkers of varying lengths and sequences. Due to their intrinsic flexibility, these linkers provide proteins a subtle way to modulate interactions and explore a wide range of conformational space. In the present study, we are seeking to understand the effect of the flexibility and dynamics of the linker involved in the STAM2 UIM-SH3 dual domain protein with respect to molecular recognition. We have engineered several constructs of UIM-SH3 with different length linkers or domain deletion. By means of SAXS and NMR experiments, we have shown that the modification of the linker modifies the flexibility and the dynamics of UIM-SH3. Indeed, the global tumbling of both the UIM and SH3 domain is different but not independent from each other while the length of the linker has an impact on the ps-ns time scale dynamics of the respective domains. Finally, the modification of the flexibility and dynamics of the linker has a drastic effect on the interaction of UIM-SH3 with Lys63-linked diubiquitin with a roughly eight-time weaker dissociation constant.
机译:多结构域蛋白代表了广泛的蛋白结构,并参与了各种相互作用。可以将它们视为以不同方式组装并通过不同长度和顺序的连接器进行连接的模块化构件。由于其固有的灵活性,这些接头为蛋白质提供了微妙的方式来调节相互作用并探索各种构象空间。在本研究中,我们正在寻求了解STAM2 UIM-SH3双结构域蛋白中涉及的接头的柔性和动力学对分子识别的影响。我们设计了几种具有不同长度接头或结构域缺失的UIM-SH3构建体。通过SAXS和NMR实验,我们已经表明,对接头的修饰会改变UIM-SH3的柔韧性和动力学。实际上,UIM和SH3域的全局翻滚是不同的,但彼此之间并不独立,而链接器的长度会影响各个域的ps-ns时标动态。最后,接头的柔性和动力学的改变对UIM-SH3与Lys63连接的双泛素的相互作用具有显着的影响,其解离常数大约弱八倍。

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