Researcher profile

Elizabeth J. Stewart

Elizabeth J. Stewart contributes to research discovery and scholarly infrastructure.

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Published work

2 published item(s)

preprint2026arXiv

A geometry-dependent, force balance-driven model of Staphylococcus epidermidis biofilm cell cluster detachment

Biofilms, bacteria cells surrounded by a self-produced polymeric matrix, are common on medical devices and lead to many hospital infections. The biofilm lifecycle includes disassembly and dispersion, where bacteria clusters detach from the biofilm, circulate in the bloodstream, and potentially colonize secondary infection sites. Existing models often simplify detachment to a function of biofilm thickness or extracellular polymeric substance (EPS) density, without tracking properties of detached clusters that impact their biological fate, including cluster size and morphology. Addressing this gap, our detachment model accounts for drag and adhesion in tagged sections of the biofilm determined by the cluster geometry and local arrangement of bacteria and EPS. A stickiness parameter controls local EPS adhesion strength, which is modulated to disrupt (or compromise) EPS biomass. We specifically model the detachment of clusters from a Staphylococcus epidermidis biofilm grown for 24 hours. Experimental data for biofilm microstructural features are utilized to benchmark the simulated biofilm, which is then subjected to different EPS disruption levels. We examine parameters that influence detached biofilm cell cluster frequency, size, and shape, providing mechanistic insights into how compromised EPS influences detachment dynamics. This integrated modeling framework is a significant advance in the predictive capabilities for biofilm detachment processes.

preprint2013arXiv

Spatially Heterogeneous Biofilm Simulations using an Immersed Boundary Method with Lagrangian Nodes Defined by Bacterial Locations

In this work we consider how surface-adherent bacterial biofilm communities respond in flowing systems. We simulate the fluid-structure interaction and separation process using the immersed boundary method. In these simulations we model and simulate different density and viscosity values of the biofilm than that of the surrounding fluid. The simulation also includes breakable springs connecting the bacteria in the biofilm. This allows the inclusion of erosion and detachment into the simulation. We use the incompressible Navier-Stokes (N-S) equations to describe the motion of the flowing fluid. We discretize the fluid equations using finite differences and use a geometric multigrid method to solve the resulting equations at each time step. The use of multigrid is necessary because of the dramatically different densities and viscosities between the biofilm and the surrounding fluid. We investigate and simulate the model in both two and three dimensions. Our method differs from previous attempts of using IBM for modeling biofilm/flow interactions in the following ways: the density and viscosity of the biofilm can differ from the surrounding fluid, and the Lagrangian node locations correspond to experimentally measured bacterial cell locations from 3D images taken of Staphylococcus epidermidis in a biofilm.