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半胱氨酸在 R3 tau 肽中调节血红素结合和反应性。

Cysteine in the R3 Tau Peptide Modulates Hemin Binding and Reactivity.

机构信息

Dipartimento di Chimica, Università di Pavia, Via Taramelli 12, Pavia 27100, Italy.

Dipartimento di Biologia e Biotecnologie, Università di Pavia, Via Ferrata 9, Pavia 27100, Italy.

出版信息

Inorg Chem. 2024 Jul 1;63(26):11986-12002. doi: 10.1021/acs.inorgchem.4c00727. Epub 2024 Jun 19.

DOI:10.1021/acs.inorgchem.4c00727
PMID:38897979
Abstract

Tau is a neuronal protein involved in axonal stabilization; however under pathological conditions, it triggers the deposition of insoluble neurofibrillary tangles, which are one of the biomarkers for Alzheimer's disease. The factors that might influence the fibrillation process are two cysteine residues in two pseudorepetitive regions, called R2 and R3, which can modulate protein-protein interaction via disulfide cross-linking; an increase of reactive oxygen species affecting the post-translational modification of tau; and cytotoxic levels of metals, especially ferric-heme (hemin), in hemolytic processes. Herein, we investigated how the cysteine-containing R3 peptide (R3C) and its Cys→Ala mutant (R3A) interact with hemin and how their binding affects the oxidative damage of the protein. The calculated binding constants are remarkably higher for the hemin-R3C complex (Log = 5.90; Log = 5.80) with respect to R3A (Log = 4.44; Log < 2), although NMR and CD investigations excluded the direct binding of cysteine as an iron axial ligand. Both peptides increase the peroxidase-like activity of hemin toward catecholamines and phenols, with a double catalytic efficiency detected for hemin-R3C systems. Moreover, the presence of cysteine significantly alters the susceptibility of R3 toward oxidative modifications, easily resulting in peptide dopamination and formation of cross-linked S-S derivatives.

摘要

tau 是一种参与轴突稳定的神经元蛋白;然而,在病理条件下,它会触发不溶性神经原纤维缠结的沉积,这是阿尔茨海默病的生物标志物之一。可能影响纤维形成过程的因素有两个半胱氨酸残基,位于两个假重复区域,称为 R2 和 R3,它们可以通过二硫键交联调节蛋白-蛋白相互作用;活性氧物种的增加会影响 tau 的翻译后修饰;以及在溶血过程中细胞毒性水平的金属,特别是三价铁原卟啉(血红素)。在此,我们研究了含半胱氨酸的 R3 肽(R3C)及其 Cys→Ala 突变体(R3A)与血红素的相互作用方式,以及它们的结合如何影响蛋白质的氧化损伤。血红素-R3C 复合物的结合常数(Log = 5.90;Log = 5.80)明显高于 R3A(Log = 4.44;Log < 2),尽管 NMR 和 CD 研究排除了半胱氨酸作为铁轴向配体的直接结合。两种肽都增加了血红素对儿茶酚胺和酚类的过氧化物酶样活性,在血红素-R3C 体系中检测到双催化效率。此外,半胱氨酸的存在显著改变了 R3 对氧化修饰的敏感性,容易导致肽的多巴胺化和形成交联的 S-S 衍生物。

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