The actin cortex has long been hypothesized to organize membrane components, especially ordered membrane domains thought to play important functional roles at the plasma membrane. Recent developments in super-resolution fluorescence localization microscopy have enabled imaging of the actin cortex in chemically fixed cells through the use of fluorophores that spatially sample filaments at densities required to trace actin meshworks. This poster describes our ongoing efforts to quantify how actin impacts the domain structure of cell plasma membranes, utilizing these actin binding probes in conjunction with well characterized peptide markers of membrane domains. We aim to employ super-resolution imaging to validate past studies, which have characterized meshwork compartment sizes in several cell types based on diffusion data. The majority of our studies are conducted in B cells, where past work indicates that actin structure plays important roles in both antigen mediated B cell receptor signaling and in the tonic signaling that occurs in the absence of ligands. Through this approach, we explore the extent to which these signaling functions are impacted by coupling between actin and membrane domains.
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