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Spray-Dried Microparticles Containing Polymeric Micelles Encapsulating Hematoporphyrin

机译:喷雾干燥的包含含血卟啉的聚合物胶束的微粒

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摘要

The purpose of this study was to examine the properties of a new pulmonary delivery platform of microparticles containing micelles in which a therapeutic photosensitizing drug, hematoporphyrin (Hp), was encapsulated. Different poloxamers were used to form micellar Hp, and one of these, Pluronic L122-Hp, was subsequently incorporated into lactose microparticles by spray-drying. Spectral and morphological analyses were performed on both micellar Hp, and lactose microparticles containing micellar Hp (lactose-micellar Hp) before and after dissolution of the microparticles in water. Photodynamic activity of the various Hp samples were evaluated in human lung epithelial carcinoma A549 cells using a light-emitting diode (LED) device at a wavelength of 630 ± 5 nm. No significant difference was observed between micellar Hp and lactose-micellar Hp regarding the generation of singlet oxygen. The mean particle size of the microparticles was 2.3 ± 0.7 µm which is within the size range for potential lung delivery. The cellular uptake of micellar Hp and lactose-micellar Hp measured on A549 cells was at least twofold higher than those obtained with the Hp at equivalent concentrations. Micellar Hp exhibited higher cytotoxicity than Hp due to reduced formation of Hp aggregates and increased cellar uptake. The spectral properties as well as the photodynamic activity of the micellar Hp was retained when formulated into microparticles by spray-drying. Microparticles containing micelles have the potential for delivering micelle-encapsulated hydrophobic drugs in targeted therapy of pulmonary diseases.
机译:这项研究的目的是检查包含胶束的新型微粒的新型肺部输送平台的特性,其中封装了治疗性光敏药物血卟啉(Hp)。使用不同的泊洛沙姆形成胶束Hp,随后通过喷雾干燥将其中之一Pluronic L122-Hp掺入乳糖微粒中。在微粒溶解于水中之前和之后,对胶束Hp和含有胶束Hp的乳糖微粒(乳糖-胶束Hp)进行了光谱和形态分析。使用发光二极管(LED)装置在波长为630±5 nm的人肺上皮癌A549细胞中评估了各种Hp样品的光动力活性。关于单线态氧的产生,胶束Hp和乳糖-胶束Hp之间没有观察到显着差异。微粒的平均粒径为2.3±0.7微米,在潜在的肺部输送的尺寸范围内。在A549细胞上测得的胶束Hp和乳糖-胶束Hp的细胞摄取量比同等浓度的Hp至少高两倍。由于Hp聚集体的形成减少和地窖摄取增加,胶束Hp表现出比Hp更高的细胞毒性。当通过喷雾干燥配制成微粒时,胶束Hp的光谱性质以及光动力活性得以保留。含有胶束的微粒具有在肺部疾病的靶向治疗中递送胶束封装的疏水性药物的潜力。

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