Multiscale computational model of fluid flow and matrix deformation in decellularized liver

Nishii, Kenichiro; Reese, Greg; Moran, Emma; Sparks, Jessica L.

doi:10.1016/j.jmbbm.2015.11.033

Cited by 20 publications

(29 citation statements)

References 39 publications

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“…Please see Appendix-Mathematical modeling of liver biology and metastases, and cancer mechanobiology in the Supplementary Materials for an expanded overview of the prior work. Briefly, there is a rich history of mathematical modeling of liver biology, particularly liver tissue regeneration [18,19], liver fibrosis [20,21], liver toxicology [22,23], interstitial flow and mechanics in liver tissues [24][25][26][27][28][29][30]. Others have modeled the role of tissue mechanics on (mostly primary) tumor growth [31][32][33][34], including some excellent work on the role of mechanosensing in individual tumor cell proliferation [35,36], although these did not focus specifically on primary or metastatic tumor growth in liver tissues.…”

Section: Prior Mathematical Modelingmentioning

confidence: 99%

“…A detailed mathematical description of the mechanics of poroviscoelastic materials was published by [86], and the application of poroviscoelastic models to liver tissue has been demonstrated by [87][88][89] among others. The summary given here is adapted from [29,89,90]. A biphasic material consists of a linear elastic solid phase and an incompressible fluid phase, where relative motion between the two phases produces rate-dependent (i.e.…”

Section: Pve Model Overviewmentioning

confidence: 99%

“…In order to model the liver microenvironment, a three-dimensional poroviscoelastic finite element model of a quarter liver lobule ( Fig. 11) was created in Abaqus (v6.12, 3DS Dassault Systems, Waltham, MA), modified from the prior work of Nishii et al [29]. A poroviscoelastic material model was selected because this constitutive description of liver tissue mechanics has been shown to capture the viscoelastic stress-strain behavior of the solid matrix as well as pressure-driven flow of fluid through the matrix pores [29].…”

Section: Numerical Implementationmentioning

confidence: 99%

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Impact of tumor-parenchyma biomechanics on liver metastatic progression: a multi-model approach

Brodin

Nishii

Frieboes

et al. 2020

Preprint

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Colorectal carcinoma (CRC) and other cancers often metastasize to the liver in later stages of the disease, contributing significantly to patient death. While the biomechanical properties of the liver parenchyma (normal liver tissue) are known to affect primary and metastatic tumor growth in liver tissues, the role of these properties in driving or inhibiting metastatic inception remains poorly understood. This study uses a multi-model approach to study the effect of tumor-parenchyma biomechanical interactions on metastatic seeding and growth; the framework also allows investigating the impact of changing tissue biomechanics on tumor dormancy and "reawakening." We employ a detailed poroviscoelastic (PVE) model to study how tumor metastases deform the surrounding tissue, induce pressure increases, and alter interstitial fluid flow in and near the metastases. Results from these short-time simulations in detailed single hepatic lobules motivate constitutive relations and biological hypotheses for use in an agent-based model of metastatic seeding and growth in centimeter-scale tissue over months-long time scales. We find that biomechanical tumor-parenchyma interactions on shorter time scales (adhesion, repulsion, and elastic tissue deformation over minutes) and longer time scales (plastic tissue relaxation over hours) may play a key role in tumor cell seeding and growth within liver tissue. These interactions may arrest the growth of micrometastases in a dormant state and can prevent newly arriving cancer cells from establishing successful metastatic foci. Moreover, the simulations indicate ways in which dormant tumors can "reawaken" after changes in parenchymal tissue mechanical properties, as may arise during aging or following acute liver illness or injury. We conclude that the proposed modeling approach can yield insight into the role of tumor-parenchyma biomechanics in promoting liver metastatic growth, with the longer term goal of identifying conditions to clinically arrest and reverse the course of late-stage cancer. 4/25

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Section: Prior Mathematical Modelingmentioning

confidence: 99%

Section: Pve Model Overviewmentioning

confidence: 99%

Section: Numerical Implementationmentioning

confidence: 99%

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Impact of tumor-parenchyma biomechanics on liver metastatic progression: a multi-model approach

Brodin

Nishii

Frieboes

et al. 2020

Preprint

Self Cite

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“…The 3D hexagonal model of a liver lobule employed in the current work ( Fig. 1a) was directly adopted from the literature [19,26], since the geometric dimensions used for modeling liver lobules and the corresponding tracts or vessels have been discussed extensively in those works. Here the lobule was simplified as a hexagonal prism with six cylinders at the ridges to mimic its PTs, and a central cylinder at the center to replicate its CV, both of which serve as the channels for blood flow.…”

Section: Geometry Of a Liver Lobule Modelmentioning

confidence: 99%

“…The height of the regular hexagonal prism H = 0.5 mm, and the circumradius of its cross section R L = 0.25 mm. The cylinders located on the six ridges were set as PTs with radius R PT = 0.02 mm, and the central cylinder was set as CV with radius R CV = 0.03 mm [19,26]. The grey zone between the PTs and the CV represents the liver sinusoidal network ( Fig.…”

Section: Geometry Of a Liver Lobule Modelmentioning

confidence: 99%

Flow dynamics analyses of pathophysiological liver lobules using porous media theory

Lü

Feng

et al. 2017

Acta Mech. Sin.

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Blood flow inside the liver plays a key role in hepatic functions, and abnormal hemodynamics are highly correlated with liver diseases. To date, the flow field in an elementary building block of the organ, the liver lobule, is difficult to determine experimentally in humans due to its complicated structure, with radially branched microvasculature and the technical difficulties that derive from its geometric constraints. Here we established a set of 3D computational models for a liver lobule using porous media theory and analyzed its flow dynamics in normal, fibrotic, and cirrhotic lobules. Our simulations indicated that those approximations of ordinary flow in portal tracts (PTs) and the central vein, and of porous media flow in the sinusoidal network, were reasonable only for normal or fibrotic lobules. Models modified with high resistance in PTs and collateral vessels inside sinusoids were able to describe the flow features in cirrhotic lobules. Pressures, average velocities, and volume flow rates were profiled and the predictions compared well with experimental data. This study furthered our understanding of the flow dynamics features of liver lobules and the differences among normal, fibrotic, and cirrhotic lobules.

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Liver Tissue Engineering

Sparks

2017

Tissue Engineering for Artificial Organs

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Multiscale computational model of fluid flow and matrix deformation in decellularized liver

Cited by 20 publications

References 39 publications

Impact of tumor-parenchyma biomechanics on liver metastatic progression: a multi-model approach

Impact of tumor-parenchyma biomechanics on liver metastatic progression: a multi-model approach

Flow dynamics analyses of pathophysiological liver lobules using porous media theory

Liver Tissue Engineering

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