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Please use this identifier to cite or link to this item: http://hdl.handle.net/20.500.12128/299
Title: Optimizing non-invasive radiofrequency hyperthermia treatment for improving drug delivery in 4T1 mouse breast cancer model
Authors: Ware, Matthew J.
Krzykawska-Serda, Martyna
Chak-Shing Ho, Jason
Newton, Jared
Suki, Sarah
Law, Justin
Nguyen, Lam
Keshishian, Vazrik
Serda, Maciej
Taylor, Kimberly
Curley, Steven A.
Corr, Stuart J.
Keywords: hyperthermia therapy; cancer therapy; breast cancer
Issue Date: 2017
Citation: Scientific Reports, (2017), vol. 7, art. no. 43961, s. 1-9
Abstract: Interactions of high-frequency radio waves (RF) with biological tissues are currently being investigated as a therapeutic platform for non-invasive cancer hyperthermia therapy. RF delivers thermal energy into tissues, which increases intra-tumoral drug perfusion and blood-flow. Herein, we describe an optical-based method to optimize the short-term treatment schedules of drug and hyperthermia administration in a 4T1 breast cancer model via RF, with the aim of maximizing drug localization and homogenous distribution within the tumor microenvironment. This method, based on the analysis of fluorescent dyes localized into the tumor, is more time, cost and resource efficient, when compared to current analytical methods for tumor-targeting drug analysis such as HPLC and LC-MS. Alexa-Albumin 647 nm fluorphore was chosen as a surrogate for nab-paclitaxel based on its similar molecular weight and albumin driven pharmacokinetics. We found that RF hyperthermia induced a 30-40% increase in Alexa-Albumin into the tumor micro-environment 24 h after treatment when compared to non-heat treated mice. Additionally, we showed that the RF method of delivering hyperthermia to tumors was more localized and uniform across the tumor mass when compared to other methods of heating. Lastly, we provided insight into some of the factors that influence the delivery of RF hyperthermia to tumors.
URI: http://hdl.handle.net/20.500.12128/299
DOI: 10.1038/srep43961
ISSN: 2045-2322
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