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柚皮素对非酶糖基化和醛糖还原酶活性的抑制机制:结合、酶动力学和分子对接分析。

Mechanistic inhibition of non-enzymatic glycation and aldose reductase activity by naringenin: Binding, enzyme kinetics and molecular docking analysis.

机构信息

Protein Research Chair, Department of Biochemistry, College of Science, King Saud University, Riyadh, Saudi Arabia.

Department of Agricultural Microbiology, Faculty of Agricultural Sciences, Aligarh Muslim University, Aligarh, India.

出版信息

Int J Biol Macromol. 2020 Sep 15;159:87-97. doi: 10.1016/j.ijbiomac.2020.04.226. Epub 2020 May 11.

DOI:10.1016/j.ijbiomac.2020.04.226
PMID:32437808
Abstract

The aldose reductase (AR) enzyme is considered a potential target for the management of diabetic complications. In this study, we describe the binding and enzyme kinetics of AR by naringenin, a bioflavonoid present in many dietary sources. Naringenin showed an inhibitory effect on the activity of AR with an IC value of 2.6 μM in an uncompetitive manner. Binding studies confirmed that the naringenin-AR complex has high spontaneous affinity (K = 1.94-7.88 × 10) with negative ΔG° value (-5.78 kcal mol). The interaction was enthalpy driven and the microenvironment of aromatic residues of AR was also altered. Various stages of protein oxidation and glycation were also measured. Naringenin inhibited fructosamine content by approximately 31.6% at 10 μM, and at the same concentration, >93% inhibition of fluorescent advanced glycation end-products (AGEs) was achieved. There was a significant recovery in free thiol groups and carbonyl content of bovine serum albumin (BSA). Furthermore, molecular docking of naringenin with AR revealed that naringenin formed two hydrogen bonds (Asn160 and Ile260), and three Pi-Pi interactions (two with Trp20 and one with His110). This study provides molecular insight of naringenin-AR interaction and mechanism of antiglycation which may be useful in the development of inhibitors for AGEs formation.

摘要

醛糖还原酶 (AR) 被认为是糖尿病并发症管理的潜在靶点。在这项研究中,我们描述了柚皮素(一种存在于许多饮食来源中的生物类黄酮)对 AR 的结合和酶动力学。柚皮素以非竞争性方式表现出对 AR 活性的抑制作用,IC 值为 2.6 μM。结合研究证实,柚皮素-AR 复合物具有高自发亲和力(K 值为 1.94-7.88×10)和负 ΔG°值(-5.78 千卡/摩尔)。相互作用由焓驱动,并且 AR 的芳香族残基的微环境也发生了变化。还测量了蛋白质氧化和糖化的各个阶段。柚皮素在 10 μM 时可使糠胺含量抑制约 31.6%,在相同浓度下,可实现荧光性晚期糖基化终产物 (AGE) 的抑制率>93%。牛血清白蛋白 (BSA) 的游离巯基基团和羰基含量有显著恢复。此外,柚皮素与 AR 的分子对接表明,柚皮素形成了两个氢键(Asn160 和 Ile260)和三个π-π相互作用(两个与 Trp20 一个与 His110)。这项研究提供了柚皮素-AR 相互作用和抗糖化机制的分子见解,这可能对开发 AGEs 形成抑制剂有用。

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