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用于肺部持续给药的姜黄素醋酸酯纳米晶体:制备、表征及体内评价

Curcumin Acetate Nanocrystals for sustained Pulmonary Delivery: Preparation, Characterization and In Vivo Evaluation.

作者信息

Hu Xiao, Yang Fei-Fei, Wei Xiao-Lan, Yao Guang-Yin, Liu Chun-Yi, Zheng Ying, Liao Yong-Hong

出版信息

J Biomed Nanotechnol. 2017 Jan;13(1):99-09. doi: 10.1166/jbn.2017.2326.

Abstract

The main objective of this study was to test the hypothesis that inhaled nanocrystals of a highly lipophilic drug could be used as a novel approach for producing sustained pulmonary delivery. Curcumin acetate, an ester prodrug of curcumin, was utilized as a highly lipophilic model drug. Curcumin acetate was subjected to wet ball milling to produce different particle sizes of nanocrystals and microparticles, and the milled curcumin acetate was spray-dried to yield similar inhalable microparticles. Following intrapulmonary administration in rats, pharmacokinetic experiments indicated that curcumin acetate significantly extended the pulmonary absorption time by 7.2-fold compared to curcumin, possibly due to the high lipophilicity of the former. The biodistribution data showed that aerosolized curcumin acetate nanocrystals 123.7 nm in size not only prolonged pulmonary retention, with the AUC value of curcumin acetate being 7.62-fold higher than that of the microparticles 1120 nm in size, but also increased the local in vivo release rate by 3.3-fold and the local availability of converted curcumin by 25.1-fold. In addition, the improved local availability resulted in better pharmacological efficacy in a monocrotaline-induced rat model of pulmonary arterial hypertension. This study was the first to demonstrate that inhalable nanocrystals are a feasible means for the sustained pulmonary delivery of highly lipophilic drugs.

摘要

本研究的主要目的是验证以下假设

吸入高亲脂性药物的纳米晶体可作为一种新型方法用于实现肺部的持续给药。姜黄素醋酸酯作为姜黄素的酯前药,被用作高亲脂性模型药物。对姜黄素醋酸酯进行湿球磨以制备不同粒径的纳米晶体和微粒,然后将研磨后的姜黄素醋酸酯进行喷雾干燥以得到类似可吸入的微粒。在大鼠肺内给药后,药代动力学实验表明,与姜黄素相比,姜黄素醋酸酯显著延长了肺部吸收时间达7.2倍,这可能归因于前者的高亲脂性。生物分布数据显示,粒径为123.7 nm的雾化姜黄素醋酸酯纳米晶体不仅延长了肺部滞留时间,姜黄素醋酸酯的AUC值比粒径为1120 nm的微粒高7.62倍,而且还使体内局部释放率提高了3.3倍,转化后的姜黄素的局部利用率提高了25.1倍。此外,局部利用率的提高在野百合碱诱导的大鼠肺动脉高压模型中产生了更好的药理疗效。本研究首次证明可吸入纳米晶体是实现高亲脂性药物肺部持续给药的一种可行方法。

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