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首页> 外文期刊>Protein engineering design & selection: PEDS >Structure-based protein engineering efforts with a monomeric TIM variant: the importance of a single point mutation for generating an active site with suitable binding properties.
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Structure-based protein engineering efforts with a monomeric TIM variant: the importance of a single point mutation for generating an active site with suitable binding properties.

机译:基于单体TIM变体的基于结构的蛋白质工程研究:单点突变对于产生具有合适结合特性的活性位点的重要性。

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摘要

A monomeric variant of triosephosphate isomerase (TIM) with a new engineered binding groove has been characterized further. In this variant (ml8bTIM), the phosphate binding loop had been shortened, causing the binding site to be much more extended. Here, it is reported that in the V233A variant of ml8bTIM (A-TIM), three important properties of the wild-type TIM active site have been restored: (i) the structural properties of loop-7, (ii) the binding site of a conserved water molecule between loop-7 and loop-8 and (iii) the binding site of the phosphate moiety. It is shown that the active site of A-TIM can bind TIM transition state analogs and suicide inhibitors competently. It is found that the active site geometry of the A-TIM complexes is less compact and more solvent exposed, as in wild-type TIM. This correlates with the observation that the catalytic efficiency of A-TIM for interconverting the TIM substrates is too low to be detected. It is also shown that the A-TIM active site can bind compounds which do not bind to wild-type TIM and which are completely different from the normal TIM substrate, like a citrate molecule. The binding of this citrate molecule is stabilized by hydrogen bonding interactions with the new binding groove.
机译:具有新的工程结合槽的磷酸三糖异构酶(TIM)的单体变体已得到进一步表征。在此变体(ml8bTIM)中,磷酸盐结合环已缩短,导致结合位点大大延长。在此,据报道,在ml8bTIM(A-TIM)的V233A变体中,野生型TIM活性位点的三个重要特性已经恢复:(i)loop-7的结构特性,(ii)结合位点环7和环8之间的保守水分子的结构和(iii)磷酸盐部分的结合位点。结果表明,A-TIM的活性位点可以有效地结合TIM过渡态类似物和自杀抑制剂。发现,与野生型TIM一样,A-TIM复合物的活性位点几何形状更不紧密,并且更多地暴露于溶剂。这与以下观察结果相关:A-TIM用于相互转化TIM底物的催化效率太低而无法检测到。还显示出A-TIM活性位点可以结合不与野生型TIM结合并且与正常TIM底物完全不同的化合物,例如柠檬酸盐分子。该柠檬酸盐分子的结合通过与新结合槽的氢键相互作用而稳定。

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