| Literature DB >> 24862442 |
Hongzhi Qiao1, Minjie Sun1, Zhigui Su1, Ying Xie1, Minglei Chen1, Li Zong2, Yahan Gao1, Huipeng Li1, Jianping Qi3, Qun Zhao4, Xiaochen Gu5, Qineng Ping6.
Abstract
Renal fibrosis is a common progressive kidney disease, and there is a lack of efficient treatment for the condition. In this study, we designed a kidney-specific nanocomplex by forming coordination-driven assembly from catechol-derived low molecular weight chitosan (HCA-Chi), metal ions and active drug molecules. The coordination activities of various metals and ligands, cytotoxicity, immunogenicity and biodistribution of HCA-Chi were investigated. Autofluorescent doxorubicin (DOX) was selected to fabricate HCA-Chi-Cu-DOX ternary nanocomplex for investigating cellular uptake behavior, transmembrane and targeting properties. The nanodevice demonstrated satisfactory stability under normal physiological conditions and pH-responsive drug release in acidic environments. Uptake of HCA-Chi-Cu-DOX by HK-2 cells was dependent on exposure time, concentration, and temperature, and was inhibited by blockers of megalin receptor. Tissue distribution showed that HCA-Chi-Cu-DOX nanocomplex was specifically accumulated in kidney with a renal relative uptake rate (r(e)) of 25.6. When active anti-fibrosis compound emodin was installed in HCA-Chi-Zn-emodin and intravenously injected to the ureter obstructed mice, obvious attenuation of fibrotic progression was exhibited. It was concluded that HCA-Chi coordination-driven nanocomplex showed special renal targeting capacity and could be utilized to develop drug delivery systems for treating renal fibrosis.Entities:
Keywords: Catechol-derived chitosan; Coordination nanocomplex; Kidney targeting; Renal fibrosis; pH-sensitive
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Year: 2014 PMID: 24862442 DOI: 10.1016/j.biomaterials.2014.04.106
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479