| 芥子酸和米糠谷蛋白非共价相互作用的分子机制研究 |
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| 引用本文: | 梁富强,段姗姗,濮欣然,郭锐林,石嘉怿.芥子酸和米糠谷蛋白非共价相互作用的分子机制研究[J].食品工业科技,2023,44(6):128-136. |
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| 作者姓名: | 梁富强 段姗姗 濮欣然 郭锐林 石嘉怿 |
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| 作者单位: | 南京财经大学食品科学与工程学院,江苏省现代粮食流通与安全协同创新中心,江苏南京 210023 |
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| 基金项目: | 国家自然科学基金青年科学基金项目(32001702)。 |
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| 摘 要: | 为探究芥子酸(sinapic acid,SA)与米糠谷蛋白(rice bran glutelin,RBG)的非共价相互作用的动态过程及其分子机制,本文利用荧光光谱法表征了荧光猝灭机制、结合位点数及热力学参数,并进一步通过分子对接结合分子动力学模拟解析了SA与RBG相互作用的动态过程和分子机制。结果表明,SA以静态猝灭的方式猝灭RBG蛋白的内源荧光形成复合物,结合位点数约为1。两者的结合是自发行为,疏水相互作用是主要驱动力。分子对接发现RBG上存在5个潜在结合位点。进一步的分子动力学模拟表明SA不仅稳定结合在C2位点,而且表现出最低的结合自由能,是最可能的结合位点。蛋白质回旋半径、均方根位移和均方根偏差分析进一步证实了SA与RBG结合的稳定性。结合自由能分解和相互作用分析从蛋白和小分子结构两个角度揭示了6个关键氨基酸(Ile131、Ile90、Gln261、Trp149、Tyr151及Tyr102)和SA的甲氧基对SA与RBG的结合具有重要作用。研究结果为SA-RBG复合物作为功能性食品配料的应用开发提供了理论基础。
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| 关 键 词: | 米糠 谷蛋白 芥子酸 相互作用 分子模拟 |
| 收稿时间: | 2022-10-26 |
Molecular Mechanism Underlying the Non-covalent Interaction between Sinapic Acid and Rice Bran Glutelin |
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| LIANG Fuqiang,DUAN Shanshan,PU Xinran,GUO Ruilin,SHI Jiayi.Molecular Mechanism Underlying the Non-covalent Interaction between Sinapic Acid and Rice Bran Glutelin[J].Science and Technology of Food Industry,2023,44(6):128-136. |
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| Authors: | LIANG Fuqiang DUAN Shanshan PU Xinran GUO Ruilin SHI Jiayi |
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| Affiliation: | Collaborative Innovation Center for Modern Grain Circulation and Safety, College of Food Science and Engineering, Nanjing University of Finance and Economics, Nanjing 210023, China |
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| Abstract: | The current study aimed to explore the dynamic binding process and molecular mechanism for the non-covalent interaction between sinapic acid (SA) and rice bran glutelin (RBG). Fluorescence spectroscopy was used to investigate the mechanism of fluorescence quenching, the number of binding sites and thermodynamic parameters. Further, the binding process of complex formation and the underlying molecular mechanism were revealed by the combination of homology modeling, molecular docking and molecular dynamic simulations. Fluorescence study showed that SA quenched the intrinsic fluorescence of RBG via static mode, indicating the formation of SA-RBG complex. The number of binding site was about 1. Thermodynamic parameters suggested that the SA could bind with RBG spontaneously, which was predominately driven by hydrophobic interactions. Molecular docking revealed that there were five potent binding sites on RBG for SA. Further molecular dynamic simulation revealed that SA could not only bind stably at binding site C2 but also exhibited the lowest binding free energy, suggesting that C2 was the most favorable binding cavity among the five predicted binding sites. Furthermore, molecular dynamic simulation results including the radius of gyrate, root mean square deviation and root mean square fluctuation further validated the binding stable between SA and RBG. The decomposition of binding free energy to per amino acid residue combined with binding mode analysis indicated that six key residues (including Ile131, Ile90, Trp149, Gln261, Tyr151 and Tyr102) of RBG and two methoxy groups of SA played critical roles in the binding process between SA an RBG. The above results would provide theoretical basis for the application and development of SA-RBG complex as functional ingredients. |
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