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Modeling of Nanotherapy Response as a Function of the Tumor Microenvironment: Focus on Liver Metastasis

Journal

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/fbioe.2020.01011

Keywords

liver metastasis; nanotherapy; tumor microenvironment; macrophages; mathematical modeling; computational simulation

Funding

  1. Cancer Prevention and Research Institute of Texas [CPRIT RP150611]
  2. Houston Methodist Cancer Center
  3. Dr. and Mrs. Alan Kaplan Gynecologic Cancer Research Fund
  4. National Institutes of Health/National Cancer Institute [R15CA203605]
  5. Texas A&M Engineering Experiment Station
  6. Texas A&M University Department of Biomedical Engineering

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The tumor microenvironment (TME) presents a challenging barrier for effective nanotherapy-mediated drug delivery to solid tumors. In particular for tumors less vascularized than the surrounding normal tissue, as in liver metastases, the structure of the organ itself conjures with cancer-specific behavior to impair drug transport and uptake by cancer cells. Cells and elements in the TME of hypovascularized tumors play a key role in the process of delivery and retention of anti-cancer therapeutics by nanocarriers. This brief review describes the drug transport challenges and how they are being addressed with advancedin vitro3D tissue models as well as within silicomathematical modeling. This modeling complements network-oriented techniques, which seek to interpret intra-cellular relevant pathways and signal transduction within cells and with their surrounding microenvironment. With a concerted effort integrating experimental observations with computational analyses spanning from the molecular- to the tissue-scale, the goal of effective nanotherapy customized to patient tumor-specific conditions may be finally realized.

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