Fabrication of Luteolin Nanoemulsion by Box-Behnken Design to Enhance its Oral Absorption Via Lymphatic Transport

IF 3.4 4区医学 Q2 PHARMACOLOGY & PHARMACY

AAPS PharmSciTech Pub Date : 2024-09-05 DOI:10.1208/s12249-024-02898-4

Liangxing Tu, Ju Wang, Yongbing Sun, Yang Wan

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Abstract

Intestinal lymphatic transport offers an alternative and effective way to deliver drugs, such as avoiding first-pass metabolism, enhancing oral bioavailability, and facilitating the treatment of targeted lymphoid-related diseases. However, the clinical use of luteolin (LUT) is limited by its poor water solubility and low bioavailability, and enhancing lymphatic transport by nanoemulsion may be an efficient way to enhance its oral bioavailability. The objective of this work is to prepare the luteolin nanoemulsions (LUT NEs), optimized its preparation parameters by using Box-Behnken design optimization (BBD) and evaluated it in vitro and in vivo. An Caco-2 / Raji B cell co-incubation monolayer model was established to simulate the M-cell pathway, and the differences in the transmembrane transport of LUT and NEs were compared. Cycloheximide (CHX) was utilized to establish rat chylomicron (CM) blocking model, and for investigating the influence of pharmacokinetic parameters in rats thereafter. The results showed that LUT NEs have good stability, the particle sizes were about 23.87 ± 0.57 nm. Compared with LUT suspension, The P_app of LUT NEs was enhanced for 3.5-folds, the oral bioavailability was increased by about 2.97-folds. In addition, after binding with chylomicron, the oral bioavailability of LUT NEs was decreased for about 30% (AUC _0–∞ (μg/L*h): 5.356 ± 1.144 vs 3.753 ± 0.188). These results demonstrated that NEs could enhance the oral absorption of luteolin via lymphatic transport routes.

Graphical Abstract

Abstract Image

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利用盒式贝肯设计制造木犀草素纳米乳液，通过淋巴运输增强其口服吸收。

肠道淋巴转运提供了另一种有效的给药方式，如避免首过代谢、提高口服生物利用度和促进靶向淋巴相关疾病的治疗。然而，由于叶黄素（LUT）的水溶性差、生物利用度低，其临床应用受到限制，而通过纳米乳液增强淋巴转运可能是提高其口服生物利用度的有效方法。本研究的目的是制备木犀草素纳米乳剂（LUT NEs），并通过盒-贝肯优化设计（BBD）对其制备参数进行优化，同时对其进行体外和体内评估。建立了 Caco-2 / Raji B 细胞共孵育单层模型来模拟 M 细胞通路，并比较了 LUT 和 NEs 跨膜转运的差异。利用环己亚胺（CHX）建立大鼠乳糜微粒（CM）阻断模型，并研究其后药代动力学参数对大鼠的影响。结果表明，LUT NEs 具有良好的稳定性，粒径约为 23.87 ± 0.57 nm。与 LUT 悬浮液相比，LUT NEs 的 Papp 提高了 3.5 倍，口服生物利用度提高了约 2.97 倍。此外，与乳糜微粒结合后，LUT NEs 的口服生物利用度降低了约 30%（AUC 0-∞ (μg/L*h)：5.356 ± 1.144 vs 3.753 ± 0.188）。这些结果表明，NEs 可通过淋巴转运途径促进叶黄素的口服吸收。

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来源期刊

AAPS PharmSciTech 医学-药学

CiteScore

6.80

自引率

3.00%

发文量

264

审稿时长

2.4 months

期刊介绍： AAPS PharmSciTech is a peer-reviewed, online-only journal committed to serving those pharmaceutical scientists and engineers interested in the research, development, and evaluation of pharmaceutical dosage forms and delivery systems, including drugs derived from biotechnology and the manufacturing science pertaining to the commercialization of such dosage forms. Because of its electronic nature, AAPS PharmSciTech aspires to utilize evolving electronic technology to enable faster and diverse mechanisms of information delivery to its readership. Submission of uninvited expert reviews and research articles are welcomed.