Focal Adhesion-Independent Cell Migration.

Cell migration is central to a multitude of physiological processes, including embryonic development, immune surveillance, and wound healing, and deregulated migration is key to cancer dissemination. Decades of investigations have uncovered many of the molecular and physical mechanisms underlying cell migration. Together with protrusion extension and cell body retraction, adhesion to the substrate via specific focal adhesion points has long been considered an essential step in cell migration. Although this is true for cells moving on two-dimensional substrates, recent studies have demonstrated that focal adhesions are not required for cells moving in three dimensions, in which confinement is sufficient to maintain a cell in contact with its substrate. Here, we review the investigations that have led to challenging the requirement of specific adhesions for migration, discuss the physical mechanisms proposed for cell body translocation during focal adhesion-independent migration, and highlight the remaining open questions for the future.

The Influence of Nucleus Mechanics in Modelling Adhesion-independent Cell Migration in Structured and Confined Environments.

Recent biological experiments (Lämmermann et al. in Nature 453(7191):51-55, 2008; Reversat et al. in Nature 7813:582-585, 2020; Balzer et al. in ASEB J Off Publ Fed Am Soc Exp Biol 26(10):4045-4056, 2012) have shown that certain types of cells are able to move in structured and confined environments even without the activation of focal adhesion. Focusing on this particular phenomenon and based on previous works (Jankowiak et al. in Math Models Methods Appl Sci 30(03):513-537, 2020), we derive a novel two-dimensional mechanical model, which relies on the following physical ingredients: the asymmetrical renewal of the actin cortex supporting the membrane, resulting in a backward flow of material; the mechanical description of the nuclear membrane and the inner nuclear material; the microtubule network guiding nucleus location; the contact interactions between the cell and the external environment. The resulting fourth order system of partial differential equations is then solved numerically to conduct a study of the qualitative effects of the model parameters, mainly those governing the mechanical properties of the nucleus and the geometry of the confining structure. Coherently with biological observations, we find that cells characterized by a stiff nucleus are unable to migrate in channels that can be crossed by cells with a softer nucleus. Regarding the geometry, cell velocity and ability to migrate are influenced by the width of the channel and the wavelength of the external structure. Even though still preliminary, these results may be potentially useful in determining the physical limit of cell migration in confined environments and in designing scaffolds for tissue engineering.