Clodronate-loaded liposomal and fibroblast-derived exosomal hybrid system for enhanced drug delivery to pulmonary fibrosis

肺纤维化 任天堂 药物输送 医学 成纤维细胞 外体 癌症研究 特发性肺纤维化 脂质体 纤维化 靶向给药 药理学 微泡 材料科学 免疫学 病理 药品 生物 内科学 细胞培养 小RNA 纳米技术 基因 生物化学 遗传学
作者
Lingna Sun,Mingrui Fan,Dong Huang,Bingqin Li,Ruoting Xu,Feng Gao,Yanzuo Chen
出处
期刊:Biomaterials [Elsevier]
卷期号:271: 120761-120761 被引量:103
标识
DOI:10.1016/j.biomaterials.2021.120761
摘要

Pulmonary fibrosis is a rapidly progressive and fatal fibrotic lung disease with high mortality and morbidity. However, pulmonary fibrosis therapy in the clinic has been limited by poor selectivity and inefficiency of drug delivery to fibroblasts. Herein, a clodronate (CLD)-loaded liposome and fibroblast-derived exosome (EL-CLD) hybrid drug delivery system with non-specific phagocytosis inhibition and fibroblast homing properties, was designed for the treatment of pulmonary fibrosis. EL-CLD effectively depleted Kupffer cells via apoptosis by passive targeting after intravenous injection, and thus significantly reduced accumulation in the liver. Notably, the EL-CLD hybrid system preferentially accumulated in the fibrotic lung, and significantly increased penetration inside pulmonary fibrotic tissue by targeted delivery due to the specific affinity for fibroblasts of the homologous exosome. Nintedanib (NIN), an anti-fibrotic agent used to treat pulmonary fibrosis, was loaded in the EL-CLD system, and achieved a remarkable improvement in curative effects. The enhanced therapeutic efficacy of NIN was a result of enhanced pulmonary fibrotic tissue accumulation and delivery, combined with a diminished macrophage-induced inflammatory response. Hence, the EL-CLD hybrid system acts as an efficient carrier for pulmonary anti-fibrotic drug delivery and should be developed as an efficient fibroblast specific therapy.
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