| Literature DB >> 33859387 |
Siqin Chen1,2,3, Yin Zhong1,2, Wufa Fan1,2,3,4, Jiajia Xiang1,2,3, Guowei Wang1,2, Quan Zhou1,2,3, Jinqiang Wang1,2, Yu Geng1,2,3, Rui Sun1,2,3, Zhen Zhang1,2, Ying Piao1,2,3, Jianguo Wang5, Jianyong Zhuo5, Hailin Cong6, Haiping Jiang7, Jun Ling8, Zichen Li4, Dingding Yang9, Xin Yao9, Xiao Xu5, Zhuxian Zhou1,2,3, Jianbin Tang1,2, Youqing Shen10,11,12.
Abstract
Effective anticancer nanomedicines need to exhibit prolonged circulation in blood, to extravasate and accumulate in tumours, and to be taken up by tumour cells. These contrasting criteria for persistent circulation and cell-membrane affinity have often led to complex nanoparticle designs with hampered clinical translatability. Here, we show that conjugates of small-molecule anticancer drugs with the polyzwitterion poly(2-(N-oxide-N,N-diethylamino)ethyl methacrylate) have long blood-circulation half-lives and bind reversibly to cell membranes, owing to the negligible interaction of the polyzwitterion with proteins and its weak interaction with phospholipids. Adsorption of the polyzwitterion-drug conjugates to tumour endothelial cells and then to cancer cells favoured their transcytosis-mediated extravasation into tumour interstitium and infiltration into tumours, and led to the eradication of large tumours and patient-derived tumour xenografts in mice. The simplicity and potency of the polyzwitterion-drug conjugates should facilitate the design of translational anticancer nanomedicines.Entities:
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Year: 2021 PMID: 33859387 DOI: 10.1038/s41551-021-00701-4
Source DB: PubMed Journal: Nat Biomed Eng ISSN: 2157-846X Impact factor: 25.671