Each cell type, defined by its function and state, is characterized by a specific size range. Indeed, cell size within a specific cell type displays a narrow distribution that can vary from as much as several orders of magnitude between smaller cells, such as red blood cells, and large muscle cells. Interestingly, this size characteristic is essentially maintained during the life cycle of an individual and highly conserved among mammals. Altogether, these features suggest that maintaining “the right size” for a given cell could play an important role in performing its function.
The actin cytoskeleton, that can form different stable while dynamic intracellular architectures, plays a major role in the structural plasticity of cells in response to changes in shape and size. Our recent work suggests that actin networks developed within a cell scale with the actual size and volume of the cell. However, how cells adapt the turnover and organization of their numerous structures assembled from a limiting pool of actin monomers remains to be understood.
In this project, we thus propose to study the organization and dynamics of actin networks in selected cell types displaying distinct sizes. In particular, our study will focus on characterizing the impact of such networks organization/dynamics on different cellular functions such as cell migration or adaptability to environmental cues. The feedback between cytoskeletal architecture dynamics, cell size and function will also be addressed by perturbing the organization and dynamics of the actin cytoskeleton in these cells.