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首页> 外文期刊>ACS Omega >Drug-Loaded PLGA Electrospraying Porous Microspheres for the Local Therapy of Primary Lung Cancer via Pulmonary Delivery
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Drug-Loaded PLGA Electrospraying Porous Microspheres for the Local Therapy of Primary Lung Cancer via Pulmonary Delivery

机译:载药PLGA电喷雾多孔微球体通过肺部递送对原发性肺癌的局部治疗

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Nonsmall-cell lung cancer is a severe disease with high morbidity and mortality. However, the systemic administration of anticancer drugs generally leads to serious toxicity and low anti-lung cancer efficiency because of very limited drug distribution in the lung. In our previous research, we have confirmed the high anti-lung cancer effect of inhalable oridonin microparticles in spite of their long and complicated preparation process. Here, we develop a novel, simple, and quick method for preparing inhalable oridonin-loaded poly(d,l-lactic-co -glycolic)acid (PLGA) porous microspheres using the electrospraying technique. The formulation and preparation processes were screened. The electrospraying porous microspheres (EPMs) were rough, porous, and suitable for pulmonary delivery. Most of the oridonin was released from the EPMs within 20 h based on drug diffusion and via PLGA erosion. The EPMs exhibited efficient lung deposition in vitro and in vivo because of their ideal aerodynamic diameters. Chemical carcinogens were used to prepare primary lung cancer rat models by direct pulmonary delivery. The EPMs showed high anti-lung cancer effect after pulmonary delivery according to CT images and pathology. Inhibition of angiogenesis and enhancement of lung cancer cell apoptosis could be the major anticancer mechanism. Electrospraying is an efficient method for the preparation of inhalable drug-loaded porous microspheres. The oridonin-loaded EPMs are promising dry powder inhalers for the local therapy of primary lung cancer.
机译:非小细胞肺癌是一种具有高发病率和死亡率的严重疾病。然而,由于在肺中的药物分布非常有限,因此抗癌药的全身给药通常导致严重的毒性和低的抗肺癌效率。在我们之前的研究中,我们确认了可吸入的冬凌草甲素微粒尽管制备过程冗长且复杂,但仍具有很高的抗肺癌作用。在这里,我们开发了一种新颖,简单,快速的方法,利用电喷雾技术制备了可吸入的含冬凌草甲素的聚(d,l-乳酸-co-乙醇酸)酸(PLGA)多孔微球。筛选制剂和制备过程。电喷雾多孔微球(EPM)粗糙,多孔,适合肺部输送。基于药物扩散和PLGA腐蚀,大多数ordinonin在20小时内从EPM中释放出来。 EPMs具有理想的空气动力学直径,因此在体外和体内均表现出有效的肺部沉积。化学致癌物用于通过直接肺部递送制备原发性肺癌大鼠模型。根据CT图像和病理显示,EPM在肺部分娩后显示出很高的抗肺癌作用。抑制血管生成和增强肺癌细胞凋亡可能是主要的抗癌机制。电喷雾是制备可吸入药物的多孔微球的有效方法。载有冬凌草甲素的EPM有望用于局部治疗原发性肺癌的干粉吸入器。

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