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Single-species reaction-diffusion equations, such as the Fisher-KPP and Porous-Fisher equations, support travelling wave solutions that are often interpreted as simple mathematical models of biological invasion. Such travelling wave solutions are thought to play a role in various applications including development, wound healing and malignant invasion. One criticism of these single-species equations is that they do not explicitly describe interactions between the invading population and the surrounding environment. In this work we study a reaction-diffusion equation that describes malignant invasion which has been used to interpret experimental measurements describing the invasion of malignant melanoma cells into surrounding human skin tissues. This model explicitly describes how the population of cancer cells degrade the surrounding tissues, thereby creating free space into which the cancer cells migrate and proliferate to form an invasion wave of malignant tissue that is coupled to a retreating wave of skin tissue. We analyse travelling wave solutions of this model using a combination of numerical simulation, phase plane analysis and perturbation techniques. Our analysis shows that the travelling wave solutions involve a range of very interesting properties that resemble certain well-established features of both the Fisher-KPP and Porous-Fisher equations, as well as a range of novel properties that can be thought of as extensions of these well-studied single-species equations. Of particular interest is that travelling wave solutions of the invasion model are very well approximated by trajectories in the Fisher-KPP phase plane that are normally disregarded. This observation establishes a previously unnoticed link between coupled multi-species reaction diffusion models of invasion and a different class of models of invasion that involve moving boundary problems.
In this paper we analyse a previously proposed cell-based model of glioblastoma (brain tumour) growth, which is based on the assumption that the cancer cells switch phenotypes between a proliferative and motile state (Gerlee and Nelander, PLoS Comp.
How epithelial cells coordinate their polarity to form functional tissues is an open question in cell biology. Here, we characterize a unique type of polarity found in liver tissue, nematic cell polarity, which is different from vectorial cell polari
Biological invasion, whereby populations of motile and proliferative individuals lead to moving fronts that invade into vacant regions, are routinely studied using partial differential equation (PDE) models based upon the classical Fisher--KPP model.
Tumour progression has been described as a sequence of traits or phenotypes that cells have to acquire if the neoplasm is to become an invasive and malignant cancer. Although the genetic mutations that lead to these phenotypes are random, the process
Solute transport is modeled using mixture theory, applied to the nanoparticle accumulation and concentration decay in the tissue space for different vascular configurations. A comparison of a single capillary configuration (SBC) with two parallel cyl