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硫辛酸恢复锌离子与人血清白蛋白的结合。

Lipoic Acid Restores Binding of Zinc Ions to Human Serum Albumin.

作者信息

Al-Harthi Samah, Chandra Kousik, Jaremko Łukasz

机构信息

Smart Health Initiative (SHI) and Red Sea Research Center (RSRC), Bioscience Program, Biological and Environmental Science & Engineering (BESE), King Abdullah University of Science and Technology (KAUST), Thuwal, Saudi Arabia.

出版信息

Front Chem. 2022 Jul 11;10:942585. doi: 10.3389/fchem.2022.942585. eCollection 2022.

Abstract

Human serum albumin (HSA) is the main zinc(II) carrier in blood plasma. The HSA site with the strongest affinity for zinc(II), multi-metal binding site A, is disrupted by the presence of fatty acids (FAs). Therefore, the FA concentration in the blood influences zinc distribution, which may affect both normal physiological processes and a range of diseases. Based on the current knowledge of HSA's structure and its coordination chemistry with zinc(II), we investigated zinc interactions and the effect of various FAs, including lipoic acid (LA), on the protein structure, stability, and zinc(II) binding. We combined NMR experiments and isothermal titration calorimetry to examine zinc(II) binding to HSA at a sub-atomic level in a quantitative manner as well as the effect of FAs. Free HSA results indicate the existence of one high-affinity zinc(II) binding site and multiple low-affinity sites. Upon the binding of FAs to HSA, we observed a range of behaviors in terms of zinc(II) affinity, depending on the type of FA. With FAs that disrupt zinc binding, the addition of LA restores HSA's affinity for zinc ions to the levels seen with free defatted HSA, indicating the possible mechanism of LA, which is effective in the treatment of diabetes and cardiovascular diseases.

摘要

人血清白蛋白(HSA)是血浆中主要的锌(II)载体。对锌(II)亲和力最强的HSA位点,即多金属结合位点A,会因脂肪酸(FAs)的存在而被破坏。因此,血液中的脂肪酸浓度会影响锌的分布,这可能会影响正常生理过程以及一系列疾病。基于目前对HSA结构及其与锌(II)配位化学的了解,我们研究了锌的相互作用以及包括硫辛酸(LA)在内的各种脂肪酸对蛋白质结构、稳定性和锌(II)结合的影响。我们结合核磁共振实验和等温滴定量热法,以定量方式在亚原子水平上研究锌(II)与HSA的结合以及脂肪酸的影响。游离HSA的结果表明存在一个高亲和力的锌(II)结合位点和多个低亲和力位点。当脂肪酸与HSA结合时,根据脂肪酸的类型,我们观察到锌(II)亲和力方面的一系列行为。对于破坏锌结合的脂肪酸,添加硫辛酸可将HSA对锌离子的亲和力恢复到游离脱脂HSA的水平,这表明了硫辛酸在治疗糖尿病和心血管疾病方面有效的可能机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2a7a/9309503/870bfe1b4646/fchem-10-942585-g001.jpg

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