© 1997 by Institute of Mathematics and its Applications
A mathematical model for the capillary endothelial cell-extracellular matrix interactions in wound-healing angiogenesis
Centre for Mathematical Biology, Mathematical Institute 24-29 St Giles', Oxford OX1 3LB, UK
Nonlinear Systems Laboratory, Mathematics Institute, University of Warwick Coventry, CV4 7AL, UK
Centre for Mathematical Biology, Mathematical Institute 24-29 St Giles', Oxford OX1 3LB, UK
Institute for Wound Healing, Department of Dermatology, Churchill Hospital Oxford OX3 7LJ, UK
Author to whom all correspondence should be addressed. E-mail: jas{at}maths.warwick.ac.uk.
Angiogenesis, the process by which new blood capillaries grow into a tissue from surrounding parent vessels, is a key event in dermal wound healing, malignant-tumour growth, and other pathologic conditions. In wound healing, new capillaries deliver vital metabolites such as amino acids and oxygen to the cells in the wound which are involved in a complex sequence of repair processes. The key cellular constituents of these new capillaries are endothelial cells: their interactions with soluble biochemical and insoluble extracellular matrix (ECM) proteins have been well documented recently, although the biological mechanisms underlying wound-healing angiogenesis are incompletely understood. Considerable recent research, including some continuum mathematical models, have focused on the interactions between endothelial cells and soluble regulators (such as growth factors). In this work, a similar modelling framework is used to investigate the roles of the insoluble ECM substrate, of which collagen is the predominant macromolecular protein. Our model consists of a partial differential equation for the endothelial-cell density (as a function of position and time) coupled to an ordinary differential equation for the ECM density. The ECM is assumed to regulate cell movement (both random and directed) and proliferation, whereas the cells synthesize and degrade the ECM. Analysis and numerical solutions of these equations highlights the roles of these processes in wound-healing angiogenesis. A nonstandard approximation analysis yields insight into the travel ling-wave structure of the system. The model is extended to two spatial dimensions (parallel and perpendicular to the plane of the skin), for which numerical simulations are presented. The model predicts that ECM-mediated random motility and cell proliferation are key processes which drive angiogenesis and that the details of the functional dependence of these processes on the ECM density, together with the rate of ECM remodelling, determine the qualitative nature of the angiogenic response. These predictions are experimentally testable, and they may lead towards a greater understanding of the biological mechanisms involved in wound-healing angiogenesis.
Keywords: wound healing; angiogenesis; travelling waves