The hydrolytic stability of the human tubulin α 1A protein fragment – a potential reason for the role of metal ions in the development of neurodegenerative diseases†

IF 6.4 1区 化学 Q1 CHEMISTRY, INORGANIC & NUCLEAR Inorganic Chemistry Frontiers Pub Date : 2025-03-05 DOI:10.1039/D4QI03271C
Balázs Sándor, Ágnes Grenács, Gergő Zoltán Sajtos, Giuseppina Sabatino, Giuseppe Di Natale, Giuseppe Pappalardo and Katalin Várnagy
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Abstract

Alpha-tubulin proteins are recognised as key components in the process of cell division due to their role in dimerisation and polymerisation, which results in the formation of microtubules in eukaryotes; however in the context of Alzheimer's disease (AD) and other neurodegenerative diseases (NDDs), they may also play an important role, as alterations in their structure and disintegration have been observed. The present paper investigates the 189–195 region of the human tubulin α 1A protein, in the presence of essential copper(II) and zinc(II) ions and the toxic nickel(II) metal ions. The aforementioned natural protein fragment contains the –(S/T)XH– amino acid motif, whose sequences were previously identified as active sites for a metal-ion-induced, sequence-specific hydrolysis process. The solution equilibrium studies (pH-potentiometry and UV-Vis and CD spectroscopy) demonstrated that the nickel(II) and copper(II) complexes formed under physiological pH conditions exhibit enhanced thermodynamic stability. The RP-HPLC and MS studies confirmed the irreversible behaviour of the heptapeptide due to the formation of the intermediate and final products of the hydrolytic reaction, which were induced by the nickel(II) and copper(II) metal ions. In the presence of nickel(II) ions under conditions of a pH of 8.2 and a temperature of 37 °C, the kinetic parameters of the reaction were determined. The half-life value for the formation of the intermediate product was found to be 3.70 hours, while that for the formation of the final product was 73.75 hours.

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人微管蛋白α 1A蛋白片段的水解稳定性-金属离子在神经退行性疾病发展中的作用的潜在原因
α微管蛋白被认为是细胞分裂过程中的关键成分,因为它们在二聚化和聚合中起作用,从而导致真核生物中微管的形成,然而在阿尔茨海默病(AD)和其他神经退行性疾病(ND)的背景下,α微管蛋白也可能发挥重要作用,因为它们的结构和分解发生了改变。本文研究了在必需铜(II)、锌(II)和有毒镍(II)金属离子存在下,人微管蛋白α 1A蛋白的189-195区域。上述天然蛋白片段含有- (S/T)XH -氨基酸基序,该序列先前被确定为金属离子诱导的序列特异性水解过程的活性位点。溶液平衡研究(pH电位、UV-Vis和CD光谱)表明,在生理pH条件下形成的金属配合物表现出增强的热力学稳定性。RP-HPLC和MS研究证实了七肽的不可逆行为,这是由于镍(II)和铜(II)金属离子诱导水解反应的中间产物和最终产物的形成。在pH为8.2、温度为37℃的条件下,在镍离子存在下,测定了反应的动力学参数。中间产物形成的半衰期为3.70小时,最终产物形成的半衰期为73.75小时。
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来源期刊
Inorganic Chemistry Frontiers
Inorganic Chemistry Frontiers CHEMISTRY, INORGANIC & NUCLEAR-
CiteScore
10.40
自引率
7.10%
发文量
587
审稿时长
1.2 months
期刊介绍: The international, high quality journal for interdisciplinary research between inorganic chemistry and related subjects
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