| Literature DB >> 30576113 |
Xinglu Huang1,2,3, Jie Zhuang4, Seung Woo Chung2,3, Buwei Huang2,5, Gilad Halpert2,3, Karina Negron2,6, Xuanrong Sun2,7,8, Jun Yang2,7, Yumin Oh2,9, Paul M Hwang4, Justin Hanes2,3,5,6,7,10, Jung Soo Suk2,3.
Abstract
Despite its central role in tumor progression and treatment resistance, poor vascularization that necessitates penetration of therapeutics through tumor extracellular matrix (ECM) constitutes a significant challenge to managing tumor hypoxia via conventional systemic treatment regimens. In addition, methods to target hypoxic tumor cells are lacking. Here, we discovered that human ferritin nanocages (FTn) possess an intrinsic ability to preferentially engage with hypoxic tumor tissues, in addition to normoxic tumor areas. We also developed a simple method of endowing FTn with spatially controlled "mosaic" surface poly(ethylene glycol) (PEG) coatings that facilitate deep penetration of FTn through ECM to reach hypoxic tumor tissues while retaining its inherent hypoxia-tropic property. Hypoxia-inhibiting agents systemically delivered via this surface-PEGylated FTn were readily accumulated in hypoxic tumor tissues, thereby providing significantly enhanced therapeutic benefits compared to the identical agents delivered in solution as a stand-alone therapy or an adjuvant to restore efficacy of conventional systemic chemotherapy.Entities:
Keywords: HIF-1α; PEGylation; drug resistance; ferritin nanocage; hypoxia; tumor penetration
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Year: 2018 PMID: 30576113 DOI: 10.1021/acsnano.8b05399
Source DB: PubMed Journal: ACS Nano ISSN: 1936-0851 Impact factor: 15.881