中国科学院机构知识库网格
Chinese Academy of Sciences Institutional Repositories Grid
Silk Fibroin-Coated Nanoagents for Acidic Lysosome Targeting by a Functional Preservation Strategy in Cancer Chemotherapy

文献类型:期刊论文

作者Tan, Mixiao; Liu, Weiwei; Liu, Fengqiu; Zhang, Wei; Gao, Hui; Cheng, Juan; Chen, Yu; Wang, Zhigang; Cao, Yang; Ran, Haitao
刊名THERANOSTICS
出版日期2019
卷号9期号:4页码:961
关键词silk fibroin coating amorphous calcium carbonate acid-responsive premature drug release cancer chemotherapy
ISSN号1838-7640
DOI10.7150/thno.30765
文献子类Article
英文摘要Background: Premature drug leakage and inefficient cellular uptake are stand out as considerable hurdles for low drug delivery efficiency in tumor chemotherapy. Thus, we established a novel drug delivery and transportation strategy mediated by biocompatible silk fibroin (SF)-coated nanoparticles to overcome these therapeutic hurdles. Methods: we first synthesised a TME-responsive biocompatible nanoplatform constructed of amorphous calcium carbonate (ACC) cores and SF shells for enhanced chemotherapy by concurrently inhibiting premature drug release, achieving lysosome-targeted explosion and locally sprayed DOX, and monitoring via PAI, which was verified both in vitro and in vivo. Results: The natural SF polymer first served as a "gatekeeper" to inhibit a drug from prematurely leaking into the circulation was demonstrated both in vitro and in vivo. Upon encountering TMEs and targeting to the acidic pH environments of lysosomes, the sensitive ACC nanoparticles were gradually degraded, eventually generating a large amount of Ca2+ and CO2, resulting in lysosomal collapse, thus preventing both the efflux of DOX from cancer cells and the protonation of DOX within the lysosome, releasing multiple hydrolytic enzyme to cytoplasm, exhibiting the optimal therapeutic dose and remarkable synergetic therapeutic performance. In particular, CO2 gas generated by the pH response of ACC nanocarriers demonstrated their imaging capability for PAI, providing the potential for quantifying and guiding drug release in targets. Conclusion: In this work, we constructed TME-responsive biocompatible NPs by coating DOX-preloaded ACC-DOX clusters with SF via a bioinspired mineralization method for efficient therapeutics. This functional lysosome-targeted preservation-strategy-based therapeutic system could provid novel insights into cancer chemotherapy.
WOS研究方向Research & Experimental Medicine
语种英语
出版者IVYSPRING INT PUBL
源URL[http://ir.sic.ac.cn/handle/331005/27428]  
专题中国科学院上海硅酸盐研究所
推荐引用方式
GB/T 7714
Tan, Mixiao,Liu, Weiwei,Liu, Fengqiu,et al. Silk Fibroin-Coated Nanoagents for Acidic Lysosome Targeting by a Functional Preservation Strategy in Cancer Chemotherapy[J]. THERANOSTICS,2019,9(4):961.
APA Tan, Mixiao.,Liu, Weiwei.,Liu, Fengqiu.,Zhang, Wei.,Gao, Hui.,...&Ran, Haitao.(2019).Silk Fibroin-Coated Nanoagents for Acidic Lysosome Targeting by a Functional Preservation Strategy in Cancer Chemotherapy.THERANOSTICS,9(4),961.
MLA Tan, Mixiao,et al."Silk Fibroin-Coated Nanoagents for Acidic Lysosome Targeting by a Functional Preservation Strategy in Cancer Chemotherapy".THERANOSTICS 9.4(2019):961.

入库方式: OAI收割

来源:上海硅酸盐研究所

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