| Literature DB >> 30368972 |
Weizhong Zhang1, Mengzhe Wang2, Wei Tang1, Ru Wen1, Shiyi Zhou1, Chaebin Lee1, Hui Wang2, Wen Jiang1, Ian Michael Delahunty1, Zipeng Zhen1, Hongmin Chen1, Matthew Chapman1, Zhanhong Wu2, Elizabeth W Howerth3, Houjian Cai4, Zibo Li2, Jin Xie1.
Abstract
Macrophages hold great potential in cancer drug delivery because they can sense chemotactic cues and home to tumors with high efficiency. However, it remains a challenge to load large amounts of therapeutics into macrophages without compromising cell functions. This study reports a silica-based drug nanocapsule approach to solve this issue. The nanocapsule consists of a drug-silica complex filling and a solid silica sheath, and it is designed to minimally release drug molecules in the early hours of cell entry. While taken up by macrophages at high rates, the nanocapsules minimally affect cell migration in the first 6-12 h, buying time for macrophages to home to tumors and release drugs in situ. In particular, it is shown that doxorubicin (Dox) as a representative drug can be loaded into macrophages up to 16.6 pg per cell using this approach. When tested in a U87MG xenograft model, intravenously (i.v.) injected Dox-laden macrophages show comparable tumor accumulation as untreated macrophages. Therapy leads to efficient tumor growth suppression, while causing little systematic toxicity. This study suggests a new cell platform for selective drug delivery, which can be readily extended to the treatment of other types of diseases.Entities:
Keywords: cancer; cell-mediated drug delivery; doxorubicin; glioblastoma; macrophages; nanoparticles
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Year: 2018 PMID: 30368972 PMCID: PMC6506271 DOI: 10.1002/adma.201805557
Source DB: PubMed Journal: Adv Mater ISSN: 0935-9648 Impact factor: 30.849