An Insight into Perfusion Anisotropy Within Solid Murine Lung Cancer Tumors

Overview

Journal Pharmaceutics

Publisher MDPI

Date 2024 Aug 29

PMID 39204354

Authors

Antonio Martino

Rossana Terracciano

Bogdan Milicevic

Miljan Milosevic

Vladimir Simic

Blake C Fallon

Yareli Carcamo-Bahena

Amber Lee R Royal

Aileen A Carcamo-Bahena

Edward Brian Butler

Richard C Willson

Milos Kojic

Carly S Filgueira

Affiliations

Soon will be listed here.

Abstract

Blood vessels are essential for maintaining tumor growth, progression, and metastasis, yet the tumor vasculature is under a constant state of remodeling. Since the tumor vasculature is an attractive therapeutic target, there is a need to predict the dynamic changes in intratumoral fluid pressure and velocity that occur across the tumor microenvironment (TME). The goal of this study was to obtain insight into perfusion anisotropy within lung tumors. To achieve this goal, we used the perfusion marker Hoechst 33342 and vascular endothelial marker CD31 to stain tumor sections from C57BL/6 mice harboring Lewis lung carcinoma tumors on their flank. Vasculature, capillary diameter, and permeability distribution were extracted at different time points along the tumor growth curve. A computational model was generated by applying a unique modeling approach based on the smeared physical fields (Kojic Transport Model, KTM). KTM predicts spatial and temporal changes in intratumoral pressure and fluid velocity within the growing tumor. Anisotropic perfusion occurs within two domains: capillary and extracellular space. Anisotropy in tumor structure causes the nonuniform distribution of pressure and fluid velocity. These results provide insights regarding local vascular distribution for optimal drug dosing and delivery to better predict distribution and duration of retention within the TME.

Citing Articles

On the generality of the finite element modeling physical fields in biological systems by the multiscale smeared concept (Kojic transport model).

Kojic M, Milosevic M, Simic V, Milicevic B, Terracciano R, Filgueira C Heliyon. 2024; 10(5):e26354.

PMID: 38434281 PMC: 10907537. DOI: 10.1016/j.heliyon.2024.e26354.

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