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Cited 4 time in webofscience Cited 4 time in scopus
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Optimising Hydrogel Release Profiles for Viro-Immunotherapy Using Oncolytic Adenovirus Expressing IL-12 and GM-CSF with Immature Dendritic Cells

Authors
Jenner, Adrianne L.Frascoli, FedericoYun, Chae-OkKim, Peter S.
Issue Date
Feb-2020
Publisher
MDPI
Keywords
sustained-release therapy; hydrogel; oncolytic virotherapy; immunotherapy; IL-12; GM-CSF; optimal control; data fitting; genetic algorithm; dendritic cells
Citation
APPLIED SCIENCES-BASEL, v.10, no.8, pp.1 - 22
Indexed
SCIE
SCOPUS
Journal Title
APPLIED SCIENCES-BASEL
Volume
10
Number
8
Start Page
1
End Page
22
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/3753
DOI
10.3390/app10082872
ISSN
2076-3417
Abstract
Sustained-release delivery systems, such as hydrogels, significantly improve cancer therapies by extending the treatment efficacy and avoiding excess wash-out. Combined virotherapy and immunotherapy (viro-immunotherapy) is naturally improved by these sustained-release systems, as it relies on the continual stimulation of the antitumour immune response. In this article, we consider a previously developed viro-immunotherapy treatment where oncolytic viruses that are genetically engineered to infect and lyse cancer cells are loaded onto hydrogels with immature dendritic cells (DCs). The time-dependent release of virus and immune cells results in a prolonged cancer cell killing from both the virus and activated immune cells. Although effective, a major challenge is optimising the release profile of the virus and immature DCs from the gel so as to obtain a minimum tumour size. Using a system of ordinary differential equations calibrated to experimental results, we undertake a novel numerical investigation of different gel-release profiles to determine the optimal release profile for this viro-immunotherapy. Using a data-calibrated mathematical model, we show that if the virus is released rapidly within the first few days and the DCs are released for two weeks, the tumour burden can be significantly decreased. We then find the true optimal gel-release kinetics using a genetic algorithm and suggest that complex profiles present unnecessary risk and that a simple linear-release model is optimal. In this work, insight is provided into a fundamental problem in the growing field of sustained-delivery systems using mathematical modelling and analysis.
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