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A computational diffusion model to study antibody transport within reconstructed tumor microenvironments

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10.1186/s12859-020-03854-2
 
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hdl:2117/341867

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Gualda Manzano, Emilio JoséMés informacióMés informacióMés informació
Marsal, Maria
Isidro, Inês
Almeida, Jaime
Document typeArticle
Defense date2020-12
Rights accessOpen Access
Attribution-NonCommercial-NoDerivs 3.0 Spain
Except where otherwise noted, content on this work is licensed under a Creative Commons license : Attribution-NonCommercial-NoDerivs 3.0 Spain
ProjectLASERLAB-EUROPE - The Integrated Initiative of European Laser Research Infrastructures (EC-H2020-654148)
Abstract
Antibodies revolutionized cancer treatment over the past decades. Despite their successfully application, there are still challenges to overcome to improve efficacy, such as the heterogeneous distribution of antibodies within tumors. Tumor microenvironment features, such as the distribution of tumor and other cell types and the composition of the extracellular matrix may work together to hinder antibodies from reaching the target tumor cells. To understand these interactions, we propose a framework combining in vitro and in silico models. We took advantage of in vitro cancer models previously developed by our group, consisting of tumor cells and fibroblasts co-cultured in 3D within alginate capsules, for reconstruction of tumor microenvironment features. Results: In this work, an experimental-computational framework of antibody transport within alginate capsules was established, assuming a purely diffusive transport, combined with an exponential saturation effect that mimics the saturation of binding sites on the cell surface. Our tumor microenvironment in vitro models were challenged with a fluorescent antibody and its transport recorded using light sheet fluorescence microscopy. Diffusion and saturation parameters of the computational model were adjusted to reproduce the experimental antibody distribution, with root mean square error under 5%. This computational framework is flexible and can simulate different random distributions of tumor microenvironment elements (fibroblasts, cancer cells and collagen fibers) within the capsule. The random distribution algorithm can be tuned to follow the general patterns observed in the experimental models. Conclusions: We present a computational and microscopy framework to track and simulate antibody transport within the tumor microenvironment that complements the previously established in vitro models platform. This framework paves the way to the development of a valuable tool to study the influence of different components of the tumor microenvironment on antibody transport.
CitationGualda Manzano, E.J. [et al.]. A computational diffusion model to study antibody transport within reconstructed tumor microenvironments. "BMC bioinformatics", Desembre 2020, vol. 21, núm. 1. 
URIhttp://hdl.handle.net/2117/341867
DOI10.1186/s12859-020-03854-2
ISSN1471-2105
Publisher versionhttps://bmcbioinformatics.biomedcentral.com/articles/10.1186/s12859-020-03854-2
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