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超越铜:探究分枝杆菌 GroEL1 HRCT 中 His 突变对 Ni(II) 配合物稳定性和形成的意义。

Beyond copper: examining the significance of His-mutations in mycobacterial GroEL1 HRCT for Ni(II) complex stability and formation.

机构信息

Faculty of Chemistry, University of Wroclaw, 50- 383 Wroclaw, Poland.

Department of Biotechnology, Chemistry and Pharmacy, University of Siena, Via A. Moro 2, 53100 Siena, Italy.

出版信息

Dalton Trans. 2024 Apr 16;53(15):6676-6689. doi: 10.1039/d4dt00011k.

Abstract

Recently, we have studied the coordination chemistry of the Cu(II)-histidine-rich C-terminal tail (HRCT) complex of the mycobacterial GroEL1 protein. The structure of this domain differs significantly compared to the well-known methionine-glycine-rich GroEL chaperonin - it was predicted that mycobacterial GroEL1 could play a significant role in the metal homeostasis of , especially copper. However, we found that this particular domain's pattern also repeats in a number of Ni(II)-binding proteins. Here, we present the studies concerning the properties of GroEL1 HRCT as a ligand for Ni(II) ions. For this purpose, we chose eight model peptides: L1 - Ac-DHDHHHGHAH, L2 - Ac-DKPAKAEDHDHHHGHAH, and 6 mutants of the latter in the pH range of 2-11. We examined the stoichiometry, stability, and spectroscopic features of copper complexes. We noticed that similar to the Cu(II)-complex, the presence of a Lys5 residue significantly increases the stability of the system. The impact of His mutations was also examined and carefully studied using NMR spectroscopy. His9 and His13 are the crucial residues for Ni(II) binding, whereas His12 has minimal relevance in complex formation.

摘要

最近,我们研究了铜(II)-组氨酸丰富的 C 端尾 (HRCT) 复合体的配位化学。与众所周知的蛋氨酸-甘氨酸丰富的 GroEL 伴侣蛋白相比,该结构域的结构差异显著-据预测,分枝杆菌 GroEL1 可能在金属稳态,尤其是铜中发挥重要作用。然而,我们发现该特定结构域的模式也在许多镍(II)结合蛋白中重复出现。在这里,我们介绍了关于 GroEL1 HRCT 作为 Ni(II)离子配体的性质的研究。为此,我们选择了 8 个模型肽:L1 - Ac-DHDHHHGHAH、L2 - Ac-DKPAKAEDHDHHHGHAH 以及后者的 6 个突变体,pH 值范围为 2-11。我们检查了铜配合物的化学计量、稳定性和光谱特性。我们注意到,类似于 Cu(II)-复合物,Lys5 残基的存在显著提高了体系的稳定性。还检查并使用 NMR 光谱仔细研究了 His 突变的影响。His9 和 His13 是 Ni(II)结合的关键残基,而 His12 在复合物形成中相关性最小。

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