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锆酞菁抑制热诱导蛋白质聚集。

Inhibition of heat-induced protein aggregation by zirconium phthalocyanines.

机构信息

Institute of Molecular Biology and Genetics, NASU, Kyiv, Ukraine.

V.I. Vernadsky Institute of General and Inorganic Chemistry, NASU, Kyiv, Ukraine.

出版信息

Proteins. 2023 Jul;91(7):890-903. doi: 10.1002/prot.26475. Epub 2023 Feb 13.

DOI:10.1002/prot.26475
PMID:36732896
Abstract

Specific proteins found in food sources tend to aggregate into fibrils under heat treatment; studying these aggregation processes and developing tools to control protein heat-induced aggregation is an active area of research. Phthalocyanine complexes are known to exhibit antiprionic and anti-fibrillogenic activity. Thus, the anti-fibrillogenic effect of a series of Zr phthalocyanines with different out-of-plane coordinated ligands, namely positively charged (PcZrLys ), negatively charged (PcZrCitr ), and group able to form disulfide bridges (PcZrS ), on the heat-induced aggregation of such proteins as BLG, insulin, and lysozyme was studied. The inhibition of reaction activity up to about 90% was observed in the presence of these compounds for all proteins. The effective concentration of the inhibitor was calculated for the compound with the highest activity (PcZrS ) to be 10.6 ± 3.6 and 7.3 ± 1.2 μM/L, respectively. Fluorescence spectroscopy studies demonstrated similar binding constants of three phthalocyanines binding with BLG globule. This is consistent with the results of molecular dynamics simulation, which imply the interaction of the globule with the tetrapyrrole macrocycle of phthalocyanine, leading to the globule stabilization. At the same time, TEM shows that in the presence of phthalocyanine PcZrS , thinner and longer fibrils were formed compared to control in all three proteins (BLG, insulin, and lysozyme). Thus, we can conclude that phthalocyanine PcZrS affects the amyloid aggregation's general mechanism, which is typical for proteins of different structures. Therefore, the phthalocyanine PcZrS is proposed as an anti-amyloidogenic agent suppressing heat-induced aggregation of proteins of different structures, making it potentially suitable for application in the food industry.

摘要

在热处理下,食物来源中的特定蛋白质往往会聚集形成纤维;研究这些聚集过程并开发控制蛋白质热诱导聚集的工具是一个活跃的研究领域。酞菁配合物已知具有抗朊病毒和抗纤维形成活性。因此,研究了一系列具有不同面外配位配体的锆酞菁(带正电荷的 PcZrLys、带负电荷的 PcZrCitr 和能够形成二硫键的 PcZrS)对 BLG、胰岛素和溶菌酶等蛋白质的热诱导聚集的抗纤维形成作用。在这些化合物的存在下,观察到所有蛋白质的反应活性抑制高达约 90%。对于活性最高的化合物(PcZrS),计算出抑制剂的有效浓度分别为 10.6±3.6 和 7.3±1.2 μM/L。荧光光谱研究表明,三种酞菁与 BLG 球蛋白具有相似的结合常数。这与分子动力学模拟的结果一致,表明球蛋白与酞菁的四吡咯大环相互作用,导致球蛋白稳定。同时,TEM 显示,与对照相比,在存在酞菁 PcZrS 的情况下,在所有三种蛋白质(BLG、胰岛素和溶菌酶)中形成的纤维更细更长。因此,我们可以得出结论,酞菁 PcZrS 影响了不同结构蛋白质的淀粉样纤维聚集的一般机制。因此,建议将酞菁 PcZrS 作为一种抗淀粉样变剂,抑制不同结构蛋白质的热诱导聚集,使其有可能适用于食品工业。

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