设计维生素D3配方:使用新型胶束递送系统的体外研究

Min Du, Chuck Chang, Xin Zhang, Yiming Zhang, Melissa J. Radford, R. Gahler, Y. Kuo, S. Wood, J. Solnier
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引用次数: 2

摘要

维生素D是一种具有重要免疫调节特性的必需营养素。作为一种脂溶性化合物,维生素D(及其D3形式)与水不混溶,这对吸收提出了挑战。在体外环境中,目前的研究表征了旨在提高吸收的维生素D3的新型胶束制剂。用于评估和比较胶束配方与非胶束配方的技术包括:冷冻SEM以确定形态;激光衍射以确定颗粒尺寸和分布;ζ电位测定颗粒的稳定性;溶解度测定以确定在水和胃肠道介质中的溶解度;和Caco-2细胞单层来确定肠道通透性。结果显示,在一种优化的胶束配方(LipoMicel®)中,具有有利的特性(颗粒尺寸在低微米范围内,平均ζ电位为−51.56±2.76 mV),并显著改善了肠道通透性。当引入Caco-2细胞时,LipoMicel的渗透性显著优于对照组(p<0.01;ANOVA)。本研究结果表明,维生素D3的新型胶束形式(LipoMicel)具有促进维生素D3吸收的潜力。因此,它可以作为一种很有前途的候选药物,用于人类的后续体内研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Designing Vitamin D3 Formulations: An In Vitro Investigation Using a Novel Micellar Delivery System
Vitamin D is an essential nutrient with important immunomodulatory properties. As a fat-soluble compound, Vitamin D (and its D3 form) is immiscible with water, which presents challenges to absorption. In an in vitro setting, the current study characterizes novel micellar formulations of Vitamin D3 designed to improve absorption. Techniques used to evaluate and compare the micellar formulations against a non-micellar formula include the following: cryo-SEM to determine morphology; laser diffraction to determine particle size and distribution; zeta potential to determine stability of the particles; solubility assays to determine solubility in water and gastrointestinal media; and Caco-2 cell monolayers to determine intestinal permeability. Results show advantageous features (particle size range in the low micrometres with an average zeta potential of −51.56 ± 2.76 mV), as well as significant improvements in intestinal permeability, in one optimized micellar formula (LipoMicel®). When introduced to Caco-2 cells, LipoMicel’s permeability was significantly better than the control (p < 0.01; ANOVA). Findings of this study suggest that the novel micellar form of Vitamin D3 (LipoMicel) has the potential to promote absorption of Vitamin D3. Thus, it can serve as a promising candidate for follow-up in vivo studies in humans.
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