食品科学 ›› 2023, Vol. 44 ›› Issue (10): 46-55.doi: 10.7506/spkx1002-6630-20220831-369

• 食品化学 • 上一篇    下一篇

莲子分离蛋白乳液荷载β-胡萝卜素的稳定性与消化性

孙乾,郑晓亮,王建一,郭泽镔   

  1. (1.福建农林大学食品科学学院,福建 福州 350000;2.福建农林大学 中爱国际合作食品物质学与结构设计研究中心,福建 福州 350000;3.福建中医药大学药学院,福建 福州 350122)
  • 出版日期:2023-05-25 发布日期:2023-06-02
  • 基金资助:
    福建省自然科学基金面上项目(2020J01559);福建省“雏鹰计划”青年拔尖人才专项(闽委人才[2021]5号)

Stability and Digestibility of Lotus Seed Protein Isolate Emulsion Loaded with β-Carotene

SUN Qian, ZHENG Xiaoliang, WANG Jianyi, GUO Zebin   

  1. (1. College of Food Science, Fujian Agriculture and Forestry University, Fuzhou 350000, China; 2. China-Ireland International Cooperation Centre for Food Material Science and Structure Design, Fujian Agriculture and Forestry University, Fuzhou 350000, China; 3. College of Medicine, Fujian University of Traditional Chinese Medicine, Fuzhou 350122, China)
  • Online:2023-05-25 Published:2023-06-02

摘要: 以莲子分离蛋白(lotus seed protein isolate,LSPI)为乳化剂制备高内相(高载量)β-胡萝卜素复合乳液(LSPI-BC),测定LSPI-BC稳定性与保留率变化,并模拟体外消化实验考察LSPI-BC在不同消化阶段变化机制。结果表明,由LSPI制备的LSPI-BC在低温下(4 ℃)具有长期稳定性,β-胡萝卜素保留率可达85%以上,但在高于25 ℃时稳定性与保留率明显降低。高温处理迫使LSPI展开并暴露疏水基团,形成空间网络结构赋予LSPI-BC热稳定性,并保护β-胡萝卜素免于更多降解。在体外模拟消化实验中,口腔阶段含有的唾液黏蛋白与高浓度离子的口腔消化液降低了液滴表面带电性与带电量并影响乳液稳定性。胃阶段因pH值作用发生絮凝或融合,电位由负值到正值,蛋白质聚集体分散。肠阶段液滴尺寸明显减小,电位绝对值升高。水解后1,1-二苯基-2-三硝基苯肼自由基清除能力明显提升。此外,游离脂肪酸随消化时间延长而逐渐释放,且在消化初始30 min释放量明显增大,在60 min时达到61.94%,说明LSPI更适合包埋活性物质,在酸性介质中保持活性物质的稳定性,延迟体外消化阶段活性物质释放并提高生物利用率(58.51%)。本研究为LSPI深度开发利用与促进脂溶性活性物质的高载量荷载缓释提供了理论基础。

关键词: 莲子分离蛋白;β-胡萝卜素;乳液稳定性;体外消化;生物利用率

Abstract: Lotus seed protein isolate (LSPI) was used as emulsifier to prepare high internal phase (high load) β-carotene-loaded emulsion (LSPI-BC). The stability and β-carotene retention rate of LSPI-BC were measured, and the mechanism of the changes in LSPI-BC at different stages of in vitro digestion was investigated. The results showed that LSPI-BC had long-term stability at low temperature (4 ℃), and the retention rate of β-carotene was over 85%. However, the stability and β-carotene retention rate of LSPI-BC decreased significantly when the temperature was above 25 ℃. High temperature treatment caused LSPI to unfold and expose hydrophobic groups, forming a spatial network structure that imparts LSPI-BC with good thermal stability and protects the β-carotene from further degradation. In the in vitro digestion experiment, salivary mucin and high concentrations of ions in the oral digestive fluid decreased the magnitude of surface charge on the droplets and then affected the stability of the emulsion. In the gastric phase, flocculation or fusion occurred due to the effect of pH, the potential changed from negative to positive, and the protein aggregates dispersed. In the intestinal phase, the droplet size decreased obviously and the absolute value of potential increased. After hydrolysis, the 1,1-diphenyl-2-picylhydrazyl (DPPH) radical scavenging ability increased significantly. In addition, free fatty acids were released gradually during simulated digestion, and the amount of free fatty acids released increased obviously in the first 30 min of digestion, and then reached 61.94% at 60 min, indicating that LSPI was more suitable for encapsulating active substances. The encapsulated active substance remained stable in acidic medium, its release was delayed during in vitro digestion and its bioavailability was increased to 58.51%. This study may provide a theoretical basis for the development and utilization of LSPI for high loading and sustained release of lipid-soluble active substances.

Key words: lotus seed isolate; β-carotene; emulsion stability; in vitro digestion; bioavailability

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