光甘草定/羟丙基-β-环糊精包合物的释放特性、黏液渗透性及细胞摄取

doi:10.7506/spkx1002-6630-20230120-155

摘要/Abstract

摘要： 将光甘草定（glabridin，GLD）用羟丙基-β-环糊精（hydroxypropyl-β-cyclodextrin，HP-β-CD）包合制备GLD/HP-β-CD包合物，以提高GLD在水中的溶解度；通过扫描电镜（scanning electron microscopy，SEM）、差示扫描量热（differential scanning calorimetry，DSC）法、傅里叶变换红外光谱（Fourier transform infrared spectroscopy，FTIR）法和分子对接分别研究包合物的形貌、包合物中GLD的存在形式、GLD与HP-β-CD的相互作用和空间构象。在此基础上，进一步采用体外模拟实验研究GLD/HP-β-CD包合物在胃、肠液条件下的溶出和释放特性；利用Transwell小室法研究GLD/HP-β-CD在黏液层中的渗透性，分子对接技术研究GLD与黏蛋白的空间构象及相互作用；采用Caco-2细胞研究GLD/HP-β-CD中GLD的小肠摄取，探讨载体HP-β-CD对GLD吸收的影响及可能机制。结果表明：GLD/HP-β-CD中GLD的包合率和载药率分别为90.03%、14.51%，载体HP-β-CD能使GLD在水中的饱和溶解度显著提高至109.36 mg/mL。SEM显示GLD/HP-β-CD固体包合物呈形状不规则的片状。DSC显示GLD在GLD/HP-β-CD包合物中以无定形非晶体结构存在；FTIR及DSC充分证明了HP-β-CD已将GLD包合在空腔内形成了包合物。分子对接显示GLD分子能够完整地进入到HP-β-CD的空腔内，与HP-β-CD之间的最佳结合能为－7.37 kcal/mol，分子间的相互作用主要靠范德华力维持。GLD经HP-β-CD包合后，在胃、肠液中1 h时的累积溶出率分别提高至GLD的15.75、12.4 倍，在连续胃、肠液中24 h时的累积释放率提高约53 倍；透过黏液层的表观渗透系数由9.24×10－9 cm/s提高至1.43×10－5 cm/s，分子对接研究表明GLD与黏蛋白MUC2分子间存在较强的相互作用；Caco-2细胞的摄取量由0.039 mg/g提高至0.349 mg/g。研究表明：GLD/HP-β-CD包合物可显著提高GLD的溶出和释放，极大改善GLD透过肠上皮表面黏液层的渗透性和肠上皮细胞的摄取，具有增强GLD吸收、提高GLD生物利用度的潜力。

关键词: 光甘草定；羟丙基-β-环糊精；溶出；包合物；释放；黏液层渗透；细胞摄取

Abstract: GLD/HP-β-CD inclusion complexes were prepared by encapsulating glabridin (GLD) with hydroxypropyl (HP) and β-cyclodextrin (β-CD) to improve the solubility of GLD in water. The morphology, the existing form of GLD, the interaction between GLD and HP-β-CD and the spatial conformation of the inclusion complexes were investigated by scanning electron microscopy (SEM), differential scanning calorimetry (DSC), Fourier transform infrared (FTIR) spectroscopy and molecular docking, respectively. Furthermore, the dissolution and release characteristics of GLD/HP-β-CD inclusion complexes were investigated in vitro in simulated gastric and intestinal fluids. The permeability of GLD/HP-β-CD through the mucus layer was studied using the Transwell method, and the spatial conformation and interaction of GLD and mucins were investigated by molecular docking. The small intestinal uptake of GLD in GLD/HP-β-CD inclusion complexes was studied using Caco-2 cells, and the effect of the vector HP-β-CD on GLD uptake and the possible underlying mechanism were investigated. The results showed that the encapsulation efficiency and drug loading of GLD in GLD/HP-β-CD were 90.03% and 14.51%, respectively, and HP-β-CD could significantly increase the saturation solubility of GLD in water to 109.36 mg/mL. SEM showed that the GLD/HP-β-CD solid inclusion complexes were irregularly flake-shaped. DSC showed that GLD in the GLD/HP-β-CD inclusion complexes was present in an amorphous non-crystalline form. FTIR and DSC fully demonstrated that HP-β-CD encapsulated GLD in the cavity to form an inclusion complex. Molecular docking showed that GLD molecules were able to completely enter the cavity of HP-β-CD, the optimal binding energy between GLD and HP-β-CD was −7.37 kcal/mol, and the interaction between molecules was mainly maintained by van der Waals force. Compared with free GLD, the cumulative dissolution rate of GLD/HP-β-CD at 1 h in simulated gastric and intestinal fluids was increased by 15.75 and 12.4 folds, respectively, and the total cumulative release rate at 24 h in simulated gastric and intestinal fluids was increased by 54 folds. The apparent permeability coefficient through the mucus layer was increased from 9.24 × 10-9 to 1.43 × 10-5 cm/s. Molecular docking showed a strong interaction between GLD and the mucin MUC2, and the uptake by Caco-2 cells was increased from 0.039 to 0.349 mg/g. The present study shows that GLD/HP-β-CD complexes can significantly increase the dissolution and release of GLD, and greatly improve the permeability of GLD through the mucus layer of the intestinal epithelial surface and the uptake of GLD by intestinal epithelial cells, thereby having the potential to enhance GLD absorption and improve the bioavailability of GLD.

Key words: glabridin; hydroxypropyl-β-cyclodextrin; dissolution; inclusion complex; release; mucus layer permeation; cellular uptake

中图分类号:

TS201.1

李德锋, 樊金玲, 姚培培, 任国艳, 杜琳, 张晓宇. 光甘草定/羟丙基-β-环糊精包合物的释放特性、黏液渗透性及细胞摄取[J]. 食品科学, 2023, 44(24): 16-25.

LI Defeng, FAN Jinling, YAO Peipei, REN Guoyan, DU Lin, ZHANG Xiaoyu. Release Characteristics, Mucus Permeability, and Cellular Uptake of Glabridin/Hydroxypropyl-β-Cyclodextrin Inclusion Complex[J]. FOOD SCIENCE, 2023, 44(24): 16-25.

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光甘草定/羟丙基-β-环糊精包合物的释放特性、黏液渗透性及细胞摄取

Release Characteristics, Mucus Permeability, and Cellular Uptake of Glabridin/Hydroxypropyl-β-Cyclodextrin Inclusion Complex

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