全反式和顺式虾青素对胰腺α-淀粉酶的抑制效果差异及其机制

doi:10.7506/spkx1002-6630-20250102-007

食品科学 ›› 2025, Vol. 46 ›› Issue (15): 35-46.doi: 10.7506/spkx1002-6630-20250102-007

全反式和顺式虾青素对胰腺α-淀粉酶的抑制效果差异及其机制

邹晓君，郑钦生，赵凯欣，冯裕杰，肖杰，贺丽苹，曹庸，刘晓娟

（华南农业大学食品学院，广东省功能食品活性物重点实验室，广东广州 510642）

出版日期:2025-08-15 发布日期:2025-07-22
基金资助:
国家自然科学基金面上项目（32172195）；广州市重点研发计划项目（SL2022B03J00806）

Differences in Inhibitory Effects and Mechanism of All-E and Z-Astaxanthin on Pancreatic α-Amylase

ZOU Xiaojun, ZHENG Qinsheng, ZHAO Kaixin, FENG Yujie, XIAO Jie, HE Liping, CAO Yong, LIU Xiaojuan

(Guangdong Provincial Key Laboratory of Nutraceuticals and Functional Foods, College of Food Science,South China Agricultural University, Guangzhou 510642, China)

Online:2025-08-15 Published:2025-07-22

摘要/Abstract

摘要： 通过光碘-乙醇初提-柱层析相结合方法制备高纯度顺式虾青素，以虾青素与降血糖关键调控α-淀粉酶相互作用为切入点，采用酶活性抑制实验、光谱技术和分子对接技术揭示虾青素异构体抑制猪胰腺α-淀粉酶（porcine pancreatic α-amylase，PPAA）活性能力的差异及其分子机制。结果表明，本实验成功制备并鉴定高纯度9-顺式（95.07%）和13-顺式（90.87%）虾青素，顺式虾青素比全反式虾青素具有更强的抑制PPAA活性效果（P＜0.05）。虾青素异构体与PPAA的相互作用均对Trp残基微环境造成轻微影响，不会明显改变蛋白构象。分子对接结果显示，虾青素异构体的结合位点均位于PPAA的催化口袋，与酶竞争性抑制剂阿卡波糖的结合位点相同，并且与酶催化中心的关键氨基酸残基Asp197、Glu233和Asp300具有相互作用，从而表明全反式和顺式虾青素通过竞争性结合酶催化位点的方式抑制PPAA活性。荧光猝灭结果表明，虾青素异构体与PPAA发生结合时均为静态猝灭。进一步研究发现，虾青素异构体与PPAA的主要相互作用力均为范德华力、氢键和疏水作用力，并且均与Glu233残基形成氢键，但顺式虾青素的氢键键长更短，表明其具有更强的氢键作用力。与此同时，与全反式相比，顺式虾青素具有更高的结合亲和力、更多的相互作用氨基酸残基和更低的热力学参数，表明其与PPAA具有更强的结合能力，使得顺式虾青素比全反式虾青素具有更强的酶活性抑制效果。研究结果有助于揭示虾青素异构体的降血糖活性差异和潜在机制，对于开发降血糖的新型功能性食品和药品具有重要的应用价值。

关键词: 虾青素, 全反式虾青素, 顺式虾青素, 胰腺α-淀粉酶, 抑制机制

Abstract: This study prepared high-purity Z-astaxanthin (Z-AST) by successive iodine-induced isomerization, ethanol extraction, and column chromatography. The interaction between AST and α-amylase as a key regulatory factor for blood sugar reduction was taken as a starting point to investigated the differences in the inhibitory activity of astaxanthin isomers against porcine pancreatic α-amylase (PPAA) and the underlying mechanism by enzyme inhibition assays, spectroscopic techniques and molecular docking. The results demonstrated that high-purity 9Z-AST (95.07%) and 13Z-AST (90.87%) were successfully prepared and identified. Z-AST exhibited a significantly stronger inhibitory effect on PPAA activity compared with all-E-AST (P < 0.05). Interaction studies revealed that the binding of astaxanthin isomers to PPAA caused only minor changes in the microenvironment of tryptophan (Trp) residues without significant alteration in protein conformation. Molecular docking analysis showed that the binding sites of astaxanthin isomers were located within the catalytic pocket of PPAA, coinciding with the binding site of the competitive inhibitor acarbose, and interacted with key amino acid residues at the enzyme’s catalytic center, namely Asp197, Glu233, and Asp300. This indicated that the inhibition of PPAA by astaxanthin isomers was competitive in nature. The fluorescence of PPAA was statically quenched after binding with astaxanthin isomers. Furthermore, the major interaction forces between PPAA and astaxanthin isomers were identified as van der Waals forces, hydrogen bonds, and hydrophobic interactions, and both isomers formed hydrogen bonds with the Glu233 residue. Notably, Z-AST exhibited shorter hydrogen bonds, indicating a stronger hydrogen bonding interaction. Additionally, Z-AST demonstrated higher binding affinity, interacted with more amino acid residues, and exhibited lower thermodynamic parameters compared with all-E-AST. This suggests that Z-AST possesses a stronger binding activity to PPAA, resulting in a more inhibition effect on the enzyme activity compared with all-E-AST. The findings contribute to the understanding of the differences in hypoglycemic activity between astaxanthin isomers and the potential mechanism, holding significant implications for the development of novel functional foods and hypoglycemic agents.

Key words: astaxanthin, all-E-astaxanthin, Z-astaxanthin, pancreatic α-amylase, inhibition mechanism

中图分类号:

TS201.2

邹晓君, 郑钦生, 赵凯欣, 冯裕杰, 肖杰, 贺丽苹, 曹庸, 刘晓娟. 全反式和顺式虾青素对胰腺α-淀粉酶的抑制效果差异及其机制[J]. 食品科学, 2025, 46(15): 35-46.

ZOU Xiaojun, ZHENG Qinsheng, ZHAO Kaixin, FENG Yujie, XIAO Jie, HE Liping, CAO Yong, LIU Xiaojuan. Differences in Inhibitory Effects and Mechanism of All-E and Z-Astaxanthin on Pancreatic α-Amylase[J]. FOOD SCIENCE, 2025, 46(15): 35-46.

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全反式和顺式虾青素对胰腺α-淀粉酶的抑制效果差异及其机制

Differences in Inhibitory Effects and Mechanism of All-E and Z-Astaxanthin on Pancreatic α-Amylase

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