| Literature DB >> 28075552 |
Ting Kang1, Qianqian Zhu1, Dan Wei2, Jingxian Feng1, Jianhui Yao1, Tianze Jiang1, Qingxiang Song3, Xunbin Wei2, Hongzhuan Chen3, Xiaoling Gao3, Jun Chen1.
Abstract
The dissemination, seeding, and colonization of circulating tumor cells (CTCs) serve as the root of distant metastasis. As a key step in the early stage of metastasis formation, colonization of CTCs in the (pre-)metastatic niche appears to be a valuable target. Evidence showed that inflammatory neutrophils possess both a CTC- and niche-targeting property by the intrinsic cell adhesion molecules on neutrophils. Inspired by this mechanism, we developed a nanosize neutrophil-mimicking drug delivery system (NM-NP) by coating neutrophils membranes on the surface of poly(latic-co-glycolic acid) nanoparticles (NPs). The membrane-associated protein cocktails on neutrophils membrane were mostly translocated to the surface of NM-NP via a nondisruptive approach, and the biobinding activity of neutrophils was highly preserved. Compared with uncoated NP, NM-NP exhibited enhanced cellular association in 4T1 cell models under shear flow in vitro, much higher CTC-capture efficiency in vivo, and improved homing to the premetastatic niche. Following loading with carfilzomib, a second generation of proteasome inhibitor, the NM-NP-based nanoformulation (NM-NP-CFZ) selectively depleted CTCs in the blood, prevented early metastasis and potentially inhibited the progress of already-formed metastasis. Our NP design can neutralize CTCs in the circulation and inhibit the formation of a metastatic niche.Entities:
Keywords: circulating tumor cells; drug delivery; metastasis prevention; neutrophil-mimicking nanoparticles; premetastatic niche
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Year: 2017 PMID: 28075552 DOI: 10.1021/acsnano.6b06477
Source DB: PubMed Journal: ACS Nano ISSN: 1936-0851 Impact factor: 15.881