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中国精品科技期刊2020
许欣,周展宏,李昆太,等. 牡蛎肽微胶囊的制备、结构表征及缓释性能[J]. 食品工业科技,2025,46(23):108−117. doi: 10.13386/j.issn1002-0306.2024120048.
引用本文: 许欣,周展宏,李昆太,等. 牡蛎肽微胶囊的制备、结构表征及缓释性能[J]. 食品工业科技,2025,46(23):108−117. doi: 10.13386/j.issn1002-0306.2024120048.
XU Xin, ZHOU Zhanhong, LI Kuntai, et al. Preparation, Structural Characterization, and Slow-release Performance of Oyster Peptide Microcapsules[J]. Science and Technology of Food Industry, 2025, 46(23): 108−117. (in Chinese with English abstract). doi: 10.13386/j.issn1002-0306.2024120048.
Citation: XU Xin, ZHOU Zhanhong, LI Kuntai, et al. Preparation, Structural Characterization, and Slow-release Performance of Oyster Peptide Microcapsules[J]. Science and Technology of Food Industry, 2025, 46(23): 108−117. (in Chinese with English abstract). doi: 10.13386/j.issn1002-0306.2024120048.

牡蛎肽微胶囊的制备、结构表征及缓释性能

Preparation, Structural Characterization, and Slow-release Performance of Oyster Peptide Microcapsules

  • 摘要: 为保持牡蛎肽(OEH)的稳定性,增强其缓释效果,以牡蛎肽为芯材,海藻酸钠(SA)为壁材,采用离子凝胶法制备牡蛎肽微胶囊。以包埋率为指标,通过单因素和正交试验对牡蛎肽单层微胶囊的制备工艺进行优化。在单层微胶囊(OEH-SA)基础上,以壳聚糖(CS)为壁材制备双层微胶囊(OEH-SA-CS)。比较OEH-SA 和OEH-SA-CS的包埋率、载药率、含水率和膨胀率,通过倒置显微镜(IM)、扫描电镜(SEM)、傅里叶红外光谱(FTIR)及X-射线衍射光谱(XRD)对OEH-SA和OEH-SA-CS进行表征,最后测定其缓释速率及缓释过程中的抗氧化活性。结果表明:OEH-SA的最优制备工艺为海藻酸钠质量分数1.5%、氯化钙质量分数3%、吐温80质量分数0.1%、固化时间20 min。在该条件下制备的微胶囊对OEH的包埋率为82.69%。通过1%壳聚糖固化制备的OEH-SA-CS经5 h体外模拟消化,释放率达52.49%,消化后对DPPH自由基和ABTS+自由基的清除率分别为23.9%和42.8%。相比于OEH-SA,OEH-SA-CS具有更好的缓释效果和更持久的抗氧化活性。本研究所采用的微胶囊制备工艺简单、包埋效果好,且制备的微胶囊在胃肠模拟消化中缓释效果显著,有利于OEH功能活性的发挥。研究结果可为牡蛎肽的高值化利用提供理论基础。

     

    Abstract: To maintain the stability of oyster peptides (OEH) and enhance their slow-release effect, oyster peptide microcapsules were prepared by ionotropic gelation method using oyster peptide as the core material and sodium alginate (SA) as the wall material. The preparation process of single-layer microcapsules (OEH-SA) was optimized using single-factor and orthogonal experiments, with encapsulation efficiency as the evaluation index. Based on the OEH-SA microcapsules, chitosan (CS) was used as an additional wall material to prepare double-layer microcapsules (OEH-SA-CS). The encapsulation efficiency, drug loading, moisture content, and swelling rate of OEH-SA and OEH-SA-CS were compared. Both microcapsules were characterized using inverted microscopy (IM), scanning electron microscopy (SEM), Fourier transform infrared spectroscopy (FTIR), and X-ray diffraction (XRD). The slow-release rate and antioxidant activity during release were also evaluated. The results showed that the optimal preparation conditions for OEH-SA were 1.5% sodium alginate, 3% calcium chloride, 0.1% Tween 80, and a curing time of 20 min, yielding an encapsulation efficiency of 82.69%. The OEH-SA-CS microcapsules prepared with 1% chitosan exhibited a release rate of 52.49% after 5 hours of in vitro simulated digestion, with DPPH and ABTS+ radical scavenging rates of 23.9% and 42.8%, respectively. Compared to OEH-SA, OEH-SA-CS exhibited a better slow-release effect and maintained a longer antioxidant activity. The microencapsulation process used in this study was simple, achieved good encapsulation efficiency, and the prepared microcapsules showed a certain slow-release effect in gastrointestinal simulated digestion, which was conducive to the functional activity of OEH. The results of this study can provide a theoretical basis for the high-value utilization of oyster peptides.

     

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