A fast platform for simulating flexible fiber suspensions applied to cell mechanics

TL;DR

This paper introduces a high-performance simulation platform for modeling large-scale fibrous structures in fluids, incorporating biophysical interactions relevant to cellular processes like cell division.

Contribution

It is the first to include many-body hydrodynamic interactions in cellular fiber assemblies, enabling realistic large-scale simulations of fiber dynamics in biological contexts.

Findings

Confinement affects the hydrodynamic mobility of microtubule asters.

The platform can simulate the positioning of the mitotic spindle in complex geometries.

Efficient parallelization allows simulation of thousands of fibers.

Abstract

We present a novel platform for the large-scale simulation of fibrous structures immersed in a Stokesian fluid and evolving under confinement or in free-space. One of the main motivations for this work is to study the dynamics of fiber assemblies within biological cells. For this, we also incorporate the key biophysical elements that determine the dynamics of these assemblies, which include the polymerization and depolymerization kinetics of fibers, their interactions with molecular motors and other objects, their flexibility, and hydrodynamic coupling. This work, to our knowledge, is the first technique to include many-body hydrodynamic interactions (HIs), and the resulting fluid flows, in cellular fiber assemblies. We use the non-local slender body theory to compute the fluid-structure interactions of the fibers and a second-kind boundary integral formulation for other rigid bodies and the confining boundary. A kernel-independent implementation of the fast multiple method is utilized for efficient evaluation of HIs. The deformation of the fibers is described by the nonlinear Euler--Bernoulli beam theory and their polymerization is modeled by the reparametrization of the dynamic equations in the appropriate non-Lagrangian frame. We use a pseudo-spectral representation of fiber positions and implicit HIs in the time-stepping to resolve large fiber deformations, and to allow time-steps not constrained by temporal stiffness or fiber-fiber interactions. The entire computational scheme is parallelized, which enables simulating assemblies of thousands of fibers. We use our method to investigate two important questions in the mechanics of cell division: (i) the effect of confinement on the hydrodynamic mobility of microtubule asters; and (ii) the dynamics of the positioning of mitotic spindle in complex cell geometries.