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The helix-turn-helix motif as an ultrafast independently folding domain: The pathway of folding of Engrailed homeodomain

机译:螺旋-转-螺旋基序作为超快速独立折叠域:Engrailed homeodomain的折叠路径

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摘要

Helices 2 and 3 of Engrailed homeodomain (EnHD) form a helix-turn-helix (HTH) motif. This common motif is believed not to fold independently, which is the characteristic feature of a motif rather than a domain. But we found that the EnHD HTH motif is monomeric and folded in solution, having essentially the same structure as in full-length protein. It had a sigmoidal thermal denaturation transition. Both native backbone and local tertiary interactions were formed concurrently at 4 x 10~5 s~(-1) at 25℃, monitored by IR and fluorescence T-jump kinetics, respectively, the same rate constant as for the fast phase in the folding of EnHD. The HTH motif, thus, is an ultrafast-folding, natural protein domain. Its independent stability and appropriate folding kinetics account for the stepwise folding of EnHD, satisfy fully the criteria for an on-pathway intermediate, and explain the changes in mechanism of folding across the homeodomain family. Experiments on mutated and engineered fragments of the parent protein with different probes allowed the assignment of the observed kinetic phases to specific events to show that EnHD is not an example of one-state downhill folding.
机译:Engrailed同源域(EnHD)的螺旋2和3形成螺旋-转-螺旋(HTH)主题。据信这种共同的基序不是独立折叠的,这是基序而不是域的特征。但是我们发现EnHD HTH基序是单体的,并在溶液中折叠,其结构与全长蛋白质基本相同。它具有S形热变性转变。 25℃下4 x 10〜5 s〜(-1)同时形成天然骨架和局部三级相互作用,分别通过IR和荧光T跃迁动力学进行监测,其速率常数与折叠中快相的速率常数相同EnHD。因此,HTH基序是超快折叠的天然蛋白质结构域。它的独立稳定性和适当的折叠动力学解释了EnHD的逐步折叠,完全满足了通路中间体的标准,并解释了同源域家族折叠机制的变化。用不同的探针对亲本蛋白的突变和工程片段进行的实验允许将观察到的动力学相分配给特定事件,从而表明EnHD不是单态下坡折叠的例子。

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