- •Contents
- •Contributors
- •Preface
- •1 Introduction, with the biological basis for cell mechanics
- •Introduction
- •The role of cell mechanics in biological function
- •Maintenance of cell shape
- •Cell migration
- •Mechanosensing
- •Stress responses and the role of mechanical forces in disease
- •Active cell contraction
- •Structural anatomy of a cell
- •The extracellular matrix and its attachment to cells
- •Transmission of force to the cytoskeleton and the role of the lipid bilayer
- •Intracellular structures
- •Overview
- •References
- •2 Experimental measurements of intracellular mechanics
- •Introduction
- •Forces to which cells are exposed in a biological context
- •Methods to measure intracellular rheology by macrorheology, diffusion, and sedimentation
- •Whole cell aggregates
- •Sedimentation of particles
- •Diffusion
- •Mechanical indentation of the cell surface
- •Glass microneedles
- •Cell poker
- •Atomic force microscopy
- •Mechanical tension applied to the cell membrane
- •Shearing and compression between microplates
- •Optical traps
- •Magnetic methods
- •Twisting of magnetized particles on the cell surface and interior
- •Passive microrheology
- •Optically detected individual probes
- •One-particle method
- •Two-particle methods
- •Dynamic light scattering and diffusing wave spectroscopy
- •Fluorescence correlation spectroscopy
- •Optical stretcher
- •Acoustic microscopy
- •Outstanding issues and future directions
- •References
- •3 The cytoskeleton as a soft glassy material
- •Introduction
- •Magnetic Twisting Cytometry (MTC)
- •Measurements of cell mechanics
- •The structural damping equation
- •Reduction of variables
- •Universality
- •Scaling the data
- •Collapse onto master curves
- •Theory of soft glassy rheology
- •What are soft glassy materials
- •Sollich’s theory of SGMs
- •Soft glassy rheology and structural damping
- •Open questions
- •Biological insights from SGR theory
- •Malleability of airway smooth muscle
- •Conclusion
- •References
- •4 Continuum elastic or viscoelastic models for the cell
- •Introduction
- •Purpose of continuum models
- •Principles of continuum models
- •Boundary conditions
- •Mechanical and material characteristics
- •Example of studied cell types
- •Blood cells: leukocytes and erythrocytes
- •Limitations of continuum model
- •Conclusion
- •References
- •5 Multiphasic models of cell mechanics
- •Introduction
- •Biphasic poroviscoelastic models of cell mechanics
- •Analysis of cell mechanical tests
- •Micropipette aspiration
- •Cells
- •Biphasic properties of the pericellular matrix
- •Indentation studies of cell multiphasic properties
- •Analysis of cell–matrix interactions using multiphasic models
- •Summary
- •References
- •6 Models of cytoskeletal mechanics based on tensegrity
- •Introduction
- •The cellular tensegrity model
- •The cellular tensegrity model
- •Do living cells behave as predicted by the tensegrity model?
- •Circumstantial evidence
- •Prestress-induced stiffening
- •Action at a distance
- •Do microtubules carry compression?
- •Summary
- •Examples of mathematical models of the cytoskeleton based on tensegrity
- •The cortical membrane model
- •Tensed cable nets
- •Cable-and-strut model
- •Summary
- •Tensegrity and cellular dynamics
- •Conclusion
- •Acknowledgement
- •References
- •7 Cells, gels, and mechanics
- •Introduction
- •Problems with the aqueous-solution-based paradigm
- •Cells as gels
- •Cell dynamics
- •Gels and motion
- •Secretion
- •Muscle contraction
- •Conclusion
- •Acknowledgement
- •References
- •8 Polymer-based models of cytoskeletal networks
- •Introduction
- •The worm-like chain model
- •Force-extension of single chains
- •Dynamics of single chains
- •Network elasticity
- •Nonlinear response
- •Discussion
- •References
- •9 Cell dynamics and the actin cytoskeleton
- •Introduction: The role of actin in the cell
- •Interaction of the cell cytoskeleton with the outside environment
- •The role of cytoskeletal structure
- •Actin mechanics
- •Actin dynamics
- •The emergence of actin dynamics
- •The intrinsic dynamics of actin
- •Regulation of dynamics by actin-binding proteins
- •Capping protein: ‘decommissioning’ the old
- •Gelsolin: rapid remodeling in one or two steps
- •β4-thymosin: accounting (sometimes) for the other half
- •Dynamic actin in crawling cells
- •Actin in the leading edge
- •Monomer recycling: the other ‘actin dynamics’
- •The biophysics of actin-based pushing
- •Conclusion
- •Acknowledgements
- •References
- •10 Active cellular protrusion: continuum theories and models
- •Cellular protrusion: the standard cartoon
- •The RIF formalism
- •Mass conservation
- •Momentum conservation
- •Boundary conditions
- •Cytoskeletal theories of cellular protrusion
- •Network–membrane interactions
- •Network dynamics near the membrane
- •Special cases of network–membrane interaction: polymerization force, brownian and motor ratchets
- •Network–network interactions
- •Network dynamics with swelling
- •Other theories of protrusion
- •Numerical implementation of the RIF formalism
- •An example of cellular protrusion
- •Protrusion driven by membrane–cytoskeleton repulsion
- •Protrusion driven by cytoskeletal swelling
- •Discussion
- •Conclusions
- •References
- •11 Summary
- •References
- •Index
3 The cytoskeleton as a soft glassy material
Jeffrey Fredberg and Ben Fabry
ABSTRACT: Using a novel method that was both quantitative and reproducible, Francis Crick and Arthur Hughes (Crick and Hughes, 1950) were the first to measure the mechanical properties inside single, living cells. They concluded their groundbreaking work with the words: “If we were compelled to suggest a model (of cell mechanics) we would propose Mother’s Work Basket – a jumble of beads and buttons of all shapes and sizes, with pins and threads for good measure, all jostling about and held together by colloidal forces.”
Thanks to advances in biochemistry and biophysics, we can now name and to a large degree characterize many of the beads and buttons, pins, and threads. These are the scores of cytoskeletal proteins, motor proteins, and their regulatory molecules. But the traditional reductionist approach – to study one molecule at a time in isolation – has so far not led to a comprehensive understanding of how cells are able to perform such exceptionally complex mechanical feats as division, locomotion, contraction, spreading, or remodeling. The question then arises, even if all of the cytoskeletal and signaling molecules were known and fully characterized, would this information be sufficient to understand how the cell orchestrates complex and highly specific mechanical functions? Or put another way, do molecular events playing out at the nanometer scale necessarily add up in a straightforward manner to account for mechanical events at the micrometer scale?
We argue here that the answer to these questions may be ‘No.’ We present a point of view that does not rely on a detailed knowledge of specific molecular functions and interactions, but instead focuses attention on dynamics of the microstructural arrangements between cytoskeletal proteins. Our thinking has been guided by recent advances in the physics of soft glassy materials. One of the more surprising findings that has come out of this approach is the discovery that, independent of molecular details, a single, measurable quantity (called the ‘noise temperature’) seems to account for transitions between fluid-like and solid-like states of the cytoskeleton. Although the interpretation and precise meaning of this noise temperature is still emerging, it appears to give a measure of the ‘jostling’ and the ‘colloidal forces’ that act within the cytoskeleton.
Introduction
Measurements of mechanical properties afford a unique window into the dynamics of protein-protein interactions within the cell, with elastic energy storage reflecting numbers of molecular interactions, energy dissipation reflecting their rate of turnover, and
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