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Structural and Electrostatic Asymmetry at the Active Site in Typical and Atypical Peroxiredoxin Dimers

机译:在典型的典型和非典型过氧杂毒二聚体中的活性位点的结构和静电不对称

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摘要

The peroxiredoxins (Prx) are ubiquitous peroxidases involved in important biological processes; however, details of their enzymatic mechanism remain elusive. To probe potential dynamics-function relationships, molecular dynamics simulations and electrostatic calculations were performed on the atypical 2-cysteine thiol peroxidase (Tpx) from Streptococcus pneumoniae and results compared to a previous study of a typical 2-cysteine Prx from Trypanosoma cruzi. The analyses indicate a commonality between both typical and atypical Prx: dynamic asymmetry. Asymmetry is observed in structure, fluctuations and active site electrostatics. Key residues, including Glu150 and Phe153, play roles in the developing asymmetry; furthermore, in the atypical 2-Cys Tpx, Glu150 exhibits conformation fluctuations suggesting involvement in a proton shuttle. The existence of a pathway of connected residues appears to propagate the asymmetry. The commonality of asymmetry and coupling pathways in both typical and atypical Prxs suggests a driving force towards dimer asymmetry as a common feature that plays a functional role in creating one active site with a lower cysteine pKa.
机译:过氧化毒素(PRX)是普遍存存的过氧化物酶,参与了重要的生物过程;然而,他们的酶促机制的细节仍然难以捉摸。为了探测潜在的动力学功能关系,对来自链球菌肺炎料的非典型2-半胱氨酸硫醇过氧化物酶(TPX)进行分子动力学模拟和静电计算,与先前的典型2-半胱氨酸PRX从锥虫瘤Cruzi进行比较。分析表示典型和非典型PRX:动态不对称之间的共性。在结构,波动和有源部位静电结构中观察到不对称性。关键残留物,包括GLU150和PHE153,在发展不对称中发挥作用;此外,在非典型2-Cys TPX中,Glu150表现出构象波动,暗示了Proton班车的参与。连接残留物的途径似乎传播不对称性。典型和非典型PRX中的不对称和偶联途径的共性表明二聚体不对称的驱动力作为在用下半胱氨酸PKA产生一个活性位点在创建一个活性位点时起着功能作用的常用特征。

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