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载有多巴胺-布地奈德纳米复合物的微粒用于肺部给药。

Poly(malic acid)-budesonide nanoconjugates embedded in microparticles for lung administration.

机构信息

Université Paris-Saclay, CNRS, Institut Galien Paris-Saclay, 91400, Orsay, France.

出版信息

Drug Deliv Transl Res. 2024 Aug;14(8):2062-2078. doi: 10.1007/s13346-024-01571-4. Epub 2024 Mar 22.

DOI:10.1007/s13346-024-01571-4
PMID:38517568
Abstract

To improve the therapeutic activity of inhaled glucocorticoids and reduce potential side effects, we designed a formulation combining the advantages of nanoparticles, which have an enhanced uptake by alveolar cells, allow targeted delivery and sustained drug release, as well as limited drug systemic passage, with those of microparticles, which display good alveolar deposition. Herein, a polymer-drug conjugate, poly(malic acid)-budesonide (PMAB), was first synthesized with either 11, 20, 33, or 43 mol% budesonide (drug:polymer from 1:8 to 3:4), the drug creating hydrophobic domains. The obtained conjugates self-assemble into nanoconjugates in water, yielding excellent drug loading of up to 73 wt%, with 80-100 nm diameters. In vitro assays showed that budesonide could be steadily released from the nanoconjugates, and the anti-inflammatory activity was preserved, as evidenced by reduced cytokine production in LPS-activated RAW 264.7 macrophages. Nanoconjugates were then embedded into microparticles through spray-drying with L-leucine, forming nano-embedded microparticles (NEMs). NEMs were produced with an aerodynamic diameter close to 1 µm and a density below 0.1 g.cm, indicative of a high alveolar deposition. NEMs spray-dried with the less hydrophobic nanoconjugates, PMAB 1:4, were readily dissolved in simulated lung fluid and were chosen for in vivo experiments to study pharmacokinetics in healthy rats. As it was released in vivo from NEMs, sustained distribution of budesonide was obtained for 48 h in lung tissue, cells, and lining fluid. With high loading rates, modulable release kinetics, and low cytotoxicity, these nanoconjugates delivered by NEMs are promising for the more efficient treatment of pulmonary inflammatory diseases.

摘要

为了提高吸入性糖皮质激素的治疗活性并降低潜在的副作用,我们设计了一种制剂,结合了纳米颗粒的优势,纳米颗粒具有增强的肺泡细胞摄取能力、靶向递送和持续药物释放,以及有限的药物全身通过性,以及微颗粒的优势,微颗粒显示出良好的肺泡沉积。在此,首次合成了聚合物-药物偶联物聚(马来酸)-布地奈德(PMAB),其布地奈德含量分别为 11、20、33 或 43 mol%(药物:聚合物从 1:8 到 3:4),药物形成疏水区。所得偶联物在水中自组装成纳米偶联物,药物载药量高达 73wt%,粒径为 80-100nm。体外试验表明,布地奈德可从纳米偶联物中稳定释放,抗炎活性得以保留,这可通过减少 LPS 激活的 RAW 264.7 巨噬细胞中细胞因子的产生来证明。然后通过喷雾干燥将纳米偶联物嵌入到微颗粒中,形成纳米嵌入微颗粒(NEMs)。NEMs 的空气动力学直径接近 1μm,密度低于 0.1g·cm-3,表明具有高的肺泡沉积。通过喷雾干燥疏水性较低的纳米偶联物 PMAB 1:4 制备 NEMs,它们易溶于模拟肺液中,并选择用于体内实验以研究健康大鼠中的药代动力学。由于它在体内从 NEMs 中释放出来,布地奈德在肺组织、细胞和衬里液中可维持 48 小时的持续分布。这些通过 NEMs 递送的纳米偶联物具有高载药量、可调节的释放动力学和低细胞毒性,为更有效地治疗肺部炎症性疾病提供了希望。

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本文引用的文献

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Design and in vitro characterization of multistage silicon-PLGA budesonide particles for inflammatory bowel disease.设计并体外鉴定多阶段硅-PLGA 布地奈德微粒用于炎症性肠病。
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Inhaled corticosteroids in COPD: friend or foe?COPD 患者的吸入性皮质类固醇:是敌是友?
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Glucocorticoid-loaded liposomes induce a pro-resolution phenotype in human primary macrophages to support chronic wound healing.载有糖皮质激素的脂质体诱导人原代巨噬细胞向促解决表型分化,以支持慢性伤口愈合。
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Budesonide nanocrystal-loaded hyaluronic acid microparticles for inhalation: In vitro and in vivo evaluation.载布地奈德纳米晶的透明质酸微球吸入剂:体外与体内评价。
Carbohydr Polym. 2018 Feb 1;181:1143-1152. doi: 10.1016/j.carbpol.2017.11.018. Epub 2017 Nov 4.
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Drug nanocarriers to treat autoimmunity and chronic inflammatory diseases.载药纳米载体治疗自身免疫和慢性炎症性疾病。
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Lungs deposition and pharmacokinetic study of submicron budesonide particles in Wistar rats intended for immediate effect in asthma.用于哮喘即时起效的亚微米布地奈德颗粒在Wistar大鼠体内的肺部沉积及药代动力学研究。
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