食品科学 ›› 2025, Vol. 46 ›› Issue (11): 40-48.doi: 10.7506/spkx1002-6630-20240828-210

• 基础研究 • 上一篇    

桑色素对胰脂肪酶的抑制作用

刘小娇,韩林,王敏,张玉红   

  1. (1.西藏自治区农牧科学院农产品开发与食品科学研究所,西藏 拉萨 850000;2.西北农林科技大学食品科学与工程学院,陕西 杨陵 712100)
  • 发布日期:2025-05-14
  • 基金资助:
    西藏特色食品资源高值化利用关键技术研发与应用示范项目(XZ202201ZD0001N)

Inhibitory Mechanism of Morin on Pancreatic Lipase

LIU Xiaojiao, HAN Lin, WANG Min, ZHANG Yuhong   

  1. (1. Institute of Food Science and Technology, Xizang Academy of Agriculture and Animal Husbandry Sciences, Lhasa 850000, China; 2. College of Food Science and Engineering, Northwest A&F University, Yangling 712100, China)
  • Published:2025-05-14

摘要: 为探究桑色素作为胰脂肪酶抑制剂的应用价值,通过体外和体内实验探究桑色素的降脂活性和作用机理。结果表明,桑色素是一种可逆的竞争性胰脂肪酶抑制剂,半抑制浓度为(0.42±0.02)mg/mL。桑色素通过疏水作用力、氢键和π-π键与胰脂肪酶活性部位中心的特征氨基酸残基相互作用,以静态机制猝灭胰脂肪酶荧光强度,并改变酶的二级构象,引起α-螺旋相对含量下降和β-折叠相对含量上升,最终抑制胰脂肪酶的催化活性。桑色素与阳性对照药物奥利司他均为竞争性抑制剂,二者联用的互作效果表现为奥利司他低质量浓度时相加,奥利司他高质量浓度时拮抗。小鼠口服猪油实验结果显示,桑色素能有效抑制6 h内小鼠血液中甘油三酯的快速上升,并且与奥利司他效果无显著差异,说明桑色素能通过抑制胰脂肪酶活性减少脂肪分解吸收,从而发挥降血脂活性。研究结果可为深入开发富含桑色素的降血脂功能食品提供理论依据。

关键词: 桑色素;胰脂肪酶;抑制活性;作用机理;甘油三酯

Abstract: In order to investigate the application value of morin as a pancreatic lipase inhibitor, we conducted in vitro and in vivo tests to assess its hypolipidemic activity and mechanism of action in this study. The results showed that morin functioned as a reversible competitive pancreatic lipase inhibitor with a half maximal inhibitory concentration value of (0.42 ± 0.02) mg/mL. Morin interacted with characteristic amino acid residues in the active center of pancreatic lipase through hydrophobic forces, hydrogen bonding, and π-π stacking, resulting in static quenching of the enzyme’s fluorescence. Meanwhile, morin altered its secondary structure, leading to decreased relative content of α-helix and increased relative content of β-sheet and ultimately inhibiting the activity of pancreatic lipase. Notably, morin and the positive control drug orlistat were both competitive inhibitors of pancreatic lipase. The combined use of these two inhibitors showed an additive effect at low concentrations of orlistat but antagonistic effect at high concentrations of orlistat. Morin inhibited the rapid rise of triglyceride in the blood of mice within 6 h following oral ingestion of lard and its effect was not significantly different from that of orlistat. This indicates that morin could reduce fat decomposition and absorption by inhibiting the activity of pancreatic lipase, thereby exerting hypolipidemic effects. The findings of this study provide a theoretical basis for the in-depth development of morin-rich lipid-lowering foods.

Key words: morin; pancreatic lipase; inhibitory activity; action mechanism; triglyceride

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