Maximum Likelihood Estimation for Single Particle, Passive Microrheology Data with Drift

Volume limitations and low yield thresholds of biological fluids have led to widespread use of passive microparticle rheology. The mean-squared-displacement (MSD) statistics of bead position time series (bead paths) are either applied directly to determine the creep compliance [Xu et al (1998)] or transformed to determine dynamic storage and loss moduli [Mason & Weitz (1995)]. A prevalent hurdle arises when there is a non-diffusive experimental drift in the data. Commensurate with the magnitude of drift relative to diffusive mobility, quantified by a P\'eclet number, the MSD statistics are distorted, and thus the path data must be "corrected" for drift. The standard approach is to estimate and subtract the drift from particle paths, and then calculate MSD statistics. We present an alternative, parametric approach using maximum likelihood estimation that simultaneously fits drift and diffusive model parameters from the path data; the MSD statistics (and consequently the compliance and dynamic moduli) then follow directly from the best-fit model. We illustrate and compare both methods on simulated path data over a range of P\'eclet numbers, where exact answers are known. We choose fractional Brownian motion as the numerical model because it affords tunable, sub-diffusive MSD statistics consistent with typical 30 second long, experimental observations of microbeads in several biological fluids. Finally, we apply and compare both methods on data from human bronchial epithelial cell culture mucus.Comment: 29 pages, 12 figure

Model Comparison and Assessment for Single Particle Tracking in Biological Fluids

State-of-the-art techniques in passive particle-tracking microscopy provide high-resolution path trajectories of diverse foreign particles in biological fluids. For particles on the order of 1 μm diameter, these paths are generally inconsistent with simple Brownian motion. Yet, despite an abundance of data confirming these findings and their wide-ranging scientific implications, stochastic modeling of the complex particle motion has received comparatively little attention. Even among posited models, there is virtually no literature on likelihood-based inference, model comparisons, and other quantitative assessments. In this article, we develop a rigorous and computationally efficient Bayesian methodology to address this gap. We analyze two of the most prevalent candidate models for 30-sec paths of 1 μm diameter tracer particles in human lung mucus: fractional Brownian motion (fBM) and a Generalized Langevin Equation (GLE) consistent with viscoelastic theory. Our model comparisons distinctly favor GLE over fBM, with the former describing the data remarkably well up to the timescales for which we have reliable information. Supplementary materials for this article are available online.Statistic