Ultrasound-mediated cavitation does not decrease the activity of small molecule, antibody or viral-based medicines

The treatment of cancer using nanomedicines is limited by the poor penetration of these potentially powerful agents into and throughout solid tumors. Externally controlled mechanical stimuli, such as the generation of cavitation-induced microstreaming using ultrasound (US), can provide a means of im...

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Autores principales: Myers, Rachel, Grundy, Megan, Rowe, Cliff, Coviello, Christian M, Bau, Luca, Erbs, Philippe, Foloppe, Johann, Balloul, Jean-Marc, Story, Colin, Coussios, Constantin C, Carlisle, Robert
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Dove Medical Press 2018
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5768183/
https://www.ncbi.nlm.nih.gov/pubmed/29391793
http://dx.doi.org/10.2147/IJN.S141557
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author Myers, Rachel
Grundy, Megan
Rowe, Cliff
Coviello, Christian M
Bau, Luca
Erbs, Philippe
Foloppe, Johann
Balloul, Jean-Marc
Story, Colin
Coussios, Constantin C
Carlisle, Robert
author_facet Myers, Rachel
Grundy, Megan
Rowe, Cliff
Coviello, Christian M
Bau, Luca
Erbs, Philippe
Foloppe, Johann
Balloul, Jean-Marc
Story, Colin
Coussios, Constantin C
Carlisle, Robert
author_sort Myers, Rachel
collection PubMed
description The treatment of cancer using nanomedicines is limited by the poor penetration of these potentially powerful agents into and throughout solid tumors. Externally controlled mechanical stimuli, such as the generation of cavitation-induced microstreaming using ultrasound (US), can provide a means of improving nanomedicine delivery. Notably, it has been demonstrated that by focusing, monitoring and controlling the US exposure, delivery can be achieved without damage to surrounding tissue or vasculature. However, there is a risk that such stimuli may disrupt the structure and thereby diminish the activity of the delivered drugs, especially complex antibody and viral-based nanomedicines. In this study, we characterize the impact of cavitation on four different agents, doxorubicin (Dox), cetuximab, adenovirus (Ad) and vaccinia virus (VV), representing a scale of sophistication from a simple small-molecule drug to complex biological agents. To achieve tight regulation of the level and duration of cavitation exposure, a “cavitation test rig” was designed and built. The activity of each agent was assessed with and without exposure to a defined cavitation regime which has previously been shown to provide effective and safe delivery of agents to tumors in preclinical studies. The fluorescence profile of Dox remained unchanged after exposure to cavitation, and the efficacy of this drug in killing a cancer cell line remained the same. Similarly, the ability of cetuximab to bind its epidermal growth factor receptor target was not diminished following exposure to cavitation. The encoding of the reporter gene luciferase within the Ad and VV constructs tested here allowed the infectivity of these viruses to be easily quantified. Exposure to cavitation did not impact on the activity of either virus. These data provide compelling evidence that the US parameters used to safely and successfully delivery nanomedicines to tumors in preclinical models do not detrimentally impact on the structure or activity of these nanomedicines.
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spelling pubmed-57681832018-02-01 Ultrasound-mediated cavitation does not decrease the activity of small molecule, antibody or viral-based medicines Myers, Rachel Grundy, Megan Rowe, Cliff Coviello, Christian M Bau, Luca Erbs, Philippe Foloppe, Johann Balloul, Jean-Marc Story, Colin Coussios, Constantin C Carlisle, Robert Int J Nanomedicine Original Research The treatment of cancer using nanomedicines is limited by the poor penetration of these potentially powerful agents into and throughout solid tumors. Externally controlled mechanical stimuli, such as the generation of cavitation-induced microstreaming using ultrasound (US), can provide a means of improving nanomedicine delivery. Notably, it has been demonstrated that by focusing, monitoring and controlling the US exposure, delivery can be achieved without damage to surrounding tissue or vasculature. However, there is a risk that such stimuli may disrupt the structure and thereby diminish the activity of the delivered drugs, especially complex antibody and viral-based nanomedicines. In this study, we characterize the impact of cavitation on four different agents, doxorubicin (Dox), cetuximab, adenovirus (Ad) and vaccinia virus (VV), representing a scale of sophistication from a simple small-molecule drug to complex biological agents. To achieve tight regulation of the level and duration of cavitation exposure, a “cavitation test rig” was designed and built. The activity of each agent was assessed with and without exposure to a defined cavitation regime which has previously been shown to provide effective and safe delivery of agents to tumors in preclinical studies. The fluorescence profile of Dox remained unchanged after exposure to cavitation, and the efficacy of this drug in killing a cancer cell line remained the same. Similarly, the ability of cetuximab to bind its epidermal growth factor receptor target was not diminished following exposure to cavitation. The encoding of the reporter gene luciferase within the Ad and VV constructs tested here allowed the infectivity of these viruses to be easily quantified. Exposure to cavitation did not impact on the activity of either virus. These data provide compelling evidence that the US parameters used to safely and successfully delivery nanomedicines to tumors in preclinical models do not detrimentally impact on the structure or activity of these nanomedicines. Dove Medical Press 2018-01-10 /pmc/articles/PMC5768183/ /pubmed/29391793 http://dx.doi.org/10.2147/IJN.S141557 Text en © 2018 Myers et al. This work is published by Dove Medical Press Limited, and licensed under a Creative Commons Attribution License The full terms of the License are available at http://creativecommons.org/licenses/by/4.0/. The license permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Original Research
Myers, Rachel
Grundy, Megan
Rowe, Cliff
Coviello, Christian M
Bau, Luca
Erbs, Philippe
Foloppe, Johann
Balloul, Jean-Marc
Story, Colin
Coussios, Constantin C
Carlisle, Robert
Ultrasound-mediated cavitation does not decrease the activity of small molecule, antibody or viral-based medicines
title Ultrasound-mediated cavitation does not decrease the activity of small molecule, antibody or viral-based medicines
title_full Ultrasound-mediated cavitation does not decrease the activity of small molecule, antibody or viral-based medicines
title_fullStr Ultrasound-mediated cavitation does not decrease the activity of small molecule, antibody or viral-based medicines
title_full_unstemmed Ultrasound-mediated cavitation does not decrease the activity of small molecule, antibody or viral-based medicines
title_short Ultrasound-mediated cavitation does not decrease the activity of small molecule, antibody or viral-based medicines
title_sort ultrasound-mediated cavitation does not decrease the activity of small molecule, antibody or viral-based medicines
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5768183/
https://www.ncbi.nlm.nih.gov/pubmed/29391793
http://dx.doi.org/10.2147/IJN.S141557
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