| Literature DB >> 30004666 |
Shawn Stapleton1, Michael Dunne2, Michael Milosevic3, Charles W Tran4, Matthew J Gold, Ali Vedadi, Trevor D Mckee, Pamela S Ohashi4, Christine Allen2, David A Jaffray1,3,5.
Abstract
Nanomedicine drug delivery systems are capable of transporting significant payloads to solid tumors. However, only a modest increase in antitumor efficacy relative to the standard of care has been observed. In this study, we demonstrate that a single dose of radiation or mild hyperthermia can substantially improve tumor uptake and distribution of nanotherapeutics, resulting in improved treatment efficacy. The delivery of nanomedicine was driven by a reduction in interstitial fluid pressure (IFP) and small perturbation of steady-state fluid flow. The transient effects on fluid dynamics in tumors with high IFP was also shown to dominate over immune cell endocytic capacity, another mechanism suspected of improving drug delivery. Furthermore, we demonstrate the specificity of this mechanism by showing that delivery of nanotherapeutics to low IFP tumors with high leukocyte infiltration does not benefit from pretreatment with radiation or heat. These results demonstrate that focusing on small perturbations to steady-state fluid dynamics, rather than large sustained effects or uncertain immune cell recruitment strategies, can impart a vulnerability to tumors with high IFP and enhance nanotherapeutic drug delivery and treatment efficacy.Entities:
Keywords: cancer; hyperthermia; image-guided drug delivery; interstitial fluid pressure; liposomes; nanomedicine; radiation
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Year: 2018 PMID: 30004666 DOI: 10.1021/acsnano.7b06301
Source DB: PubMed Journal: ACS Nano ISSN: 1936-0851 Impact factor: 15.881