Tumor Morphology and Phenotypic Evolution Driven by Selective Pressure from the Microenvironment

Anderson, Alexander R.A.; Weaver, Alissa M.; Cummings, Peter T.; Quaranta, Vito

doi:10.1016/j.cell.2006.09.042

Cited by 698 publications

(653 citation statements)

References 32 publications

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“…Direct representations of adhesion were first considered in the context of individual cell-based models (Turner & Sherratt 2002;Turner et al 2004;Grygierzec et al 2004). In recent years, this modelling approach has been developed significantly by Anderson and coworkers, in a series of sophisticated studies into the ways in which changes in cell-cell and cell-5 A c c e p t e d m a n u s c r i p t matrix adhesion interact with other aspects of the invasive phenotype (Anderson et al 2006Ramis-Conde et al 2008;Poplawski et al 2009). …”

Section: Modelling Adhesion In Invasion Processesmentioning

confidence: 99%

The impact of adhesion on cellular invasion processes in cancer and development

Painter

Armstrong

Sherratt

2010

Journal of Theoretical Biology

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In this paper we consider a simple continuous model to describe cell invasion, incorporating the effects of both cell-cell adhesion and cell-matrix adhesion, along with cell growth and proteolysis by cells of the surrounding extracellular matrix (ECM).We demonstrate that the model is capable of supporting both noninvasive and invasive tumour growth according to the relative strength of cell-cell to cell-matrix adhesion. Specifically, for sufficiently strong cell-matrix adhesion and/or sufficiently weak cell-cell adhesion, degradation of the surrounding ECM accompanied by cellmatrix adhesion pulls the cells into the surrounding ECM. We investigate the criticality of matrix heterogeneity on shaping invasion, demonstrating that a highly heterogeneous ECM can result in a "fingering" of the invasive front, echoing observations in real-life invasion processes ranging from malignant tumour growth to neural crest migration during embryonic development.

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Section: Modelling Adhesion In Invasion Processesmentioning

confidence: 99%

The impact of adhesion on cellular invasion processes in cancer and development

Painter

Armstrong

Sherratt

2010

Journal of Theoretical Biology

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“…1 The malignant phenotype imposes morbidity and mortality as the rapidly growing tumor impedes normal physiologic processes or the tumor itself inflicts physiologic changes resulting in pathologic conditions. An increased tendency to activate the clotting cascade, referred to as a procoagulant state, is common in cancer patients and portends a poor clinical outcome.…”

Section: Introductionmentioning

confidence: 99%

Thrombin induces osteosarcoma growth, a function inhibited by low molecular weight heparin in vitro and in vivo

Ichikawa

Cole

Magnussen

et al. 2011

Cancer

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BACKGROUND: Procoagulant states, leading to activation of the coagulation protease thrombin, are common in cancer and portend a poor clinical outcome. Although procoagulant states in osteosarcoma patients have been described, studies exploring osteosarcoma cells' ability to directly contribute to procoagulant activity have not been reported. This study explores the hypothesis that osteosarcoma can regulate thrombin generation and proliferate in response to thrombin, and that attenuating thrombin generation with anticoagulants can slow tumor growth. METHODS: Pathologic analysis of osteosarcoma with adjacent venous thrombus was performed. In vitro proliferation assays, cell-based coagulant activity assays, and quantification of coagulation cofactor expression were performed on human and murine osteosarcoma cell lines with varying aggressiveness. The efficacy of low molecular weight heparin (LMWH) attenuation of tumor-dependent thrombin generation and growth in vitro and in vivo was determined. RESULTS: Venous thrombi adjacent to osteosarcoma were found to harbor tumor surrounded by fibrin expressing coagulation cofactors, a finding associated with poor clinical outcome. More aggressive osteosarcoma cell lines had greater surface expression of procoagulant factors and generated more thrombin than less aggressive cell lines and were found to proliferate in response to thrombin. Treatment with LMWH reduced in vitro osteosarcoma proliferation and procoagulant activity as well as tumor growth in vivo. CONCLUSIONS: These findings suggest that elements of the coagulation cascade may play a role in and represent a pharmaceutical target to disrupt osteosarcoma growth. They also have broader implications, as they suggest that, to be effective, dosing of anticoagulants must take into account an individual tumor's capacity to generate thrombin. Cancer 2012;118:2494

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“…Frieboes et al [16,17] and Wise et al [53] have begun studying 3D tumor growth using a diffuse interface approach, while others have begun studying the tumor problem using multiphase mixture models (e.g., see [4,8], and [10]). Still others use discrete models, such as cellular automata and agents (e.g., see [1,5], and [9] for some recent examples).…”

Section: Introductionmentioning

confidence: 99%

A New Ghost Cell/Level Set Method for Moving Boundary Problems: Application to Tumor Growth

Macklin

Lowengrub

2008

J Sci Comput

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In this paper, we present a ghost cell/level set method for the evolution of interfaces whose normal velocity depend upon the solutions of linear and nonlinear quasi-steady reaction-diffusion equations with curvature-dependent boundary conditions. Our technique includes a ghost cell method that accurately discretizes normal derivative jump boundary conditions without smearing jumps in the tangential derivative; a new iterative method for solving linear and nonlinear quasisteady reaction-diffusion equations; an adaptive discretization to compute the curvature and normal vectors; and a new discrete approximation to the Heaviside function. We present numerical examples that demonstrate better than 1.5-order convergence for problems where traditional ghost cell methods either fail to converge or attain at best sub-linear accuracy. We apply our techniques to a model of tumor growth in complex, heterogeneous tissues that consists of a nonlinear nutrient equation and a pressure equation with geometry-dependent jump boundary conditions. We simulate the growth of glioblastoma (an aggressive brain tumor) into a large, 1 cm square of brain tissue that includes heterogeneous nutrient delivery and varied biomechanical characteristics (white matter, gray matter, cerebrospinal fluid, and bone), and we observe growth morphologies that are highly dependent upon the variations of the tissue characteristics-an effect observed in real tumor growth.

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Tumor Morphology and Phenotypic Evolution Driven by Selective Pressure from the Microenvironment

Cited by 698 publications

References 32 publications

The impact of adhesion on cellular invasion processes in cancer and development

The impact of adhesion on cellular invasion processes in cancer and development

Thrombin induces osteosarcoma growth, a function inhibited by low molecular weight heparin in vitro and in vivo

A New Ghost Cell/Level Set Method for Moving Boundary Problems: Application to Tumor Growth

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