Lamellipodin promotes actin assembly by clustering Ena/VASP proteins and tethering them to actin filaments

Enabled/Vasodilator (Ena/VASP) proteins promote actin filament assembly at multiple locations, including: leading edge membranes, focal adhesions, and the surface of intracellular pathogens. One important Ena/VASP regulator is the mig-10/Lamellipodin/RIAM family of adaptors that promote lamellipod formation in fibroblasts and drive neurite outgrowth and axon guidance in neurons. To better understand how MRL proteins promote actin network formation we studied the interactions between Lamellipodin (Lpd), actin, and VASP, both in vivo and in vitro. We find that Lpd binds directly to actin filaments and that this interaction regulates its subcellular localization and enhances its effect on VASP polymerase activity. We propose that Lpd delivers Ena/VASP proteins to growing barbed ends and increases their polymerase activity by tethering them to filaments. This interaction represents one more pathway by which growing actin filaments produce positive feedback to control localization and activity of proteins that regulate their assembly. Actin—the most abundant protein in most eukaryotic cells—assembles into a network of filaments that spans the length and breadth of the cell. Like the skeleton of an animal, this ‘actin cytoskeleton’ gives the cell its shape and strength, and enables the cell to actively move through its environment. To start moving, many cells begin assembling actin filaments next to the cell membrane. The growth of these filaments pushes the membrane forward and creates a two-dimensional structure called a ‘lamellipod’, which explores the space around the cell and steers its movement. The actin filaments in a lamellipod are dynamic and undergo repeated cycles of assembly and disassembly. These processes are tightly regulated by a variety of other proteins. Members of the Ena/VASP protein family, for example, collect the building blocks of an actin filament and rapidly stack them in place on the fast-growing end of a filament. The activities of Ena/VASP proteins play an especially important role in creating lamellipodial actin networks and in driving cell movement. Previous work showed that a protein called Lamellipodin binds to Ena/VASP proteins and helps recruit them to the cell membrane. However, it was unclear whether Lamellipodin could affect the activity of Ena/VASP proteins or their interaction with the actin filaments. Hansen and Mullins have now analyzed the interactions between Ena/VASP, Lamellipodin and actin. The experiments demonstrate that Lamellipodin does not simply tether Ena/VASP proteins to the membrane but also binds directly to actin filaments, via a binding site that is distinct from the site that contacts Ena/VASP. Further experiments with purified proteins revealed that Lamellipodin could interact with both actin filaments and Ena/VASP proteins at the same time. Hansen and Mullins also found that purified Lamellipodin interacted with VASP proteins to form clustered protein complexes, and that together with the tethering of actin filaments to the membrane, this clustering greatly increased VASP's ability to lengthen actin filaments. By visualizing Lamellipodin tagged with a green fluorescent protein in living cells, Hansen and Mullins then showed that its interaction with actin filaments was sufficient to localize Lamellipodin to the cell membrane. Finally, since Lamellipodin interacts with a multitude of signaling molecules in addition to Ena/VASP proteins, the next big challenge is to understand how Lamellipodin itself is regulated. Future studies could also explore how cells harness the power of the actin cytoskeleton to carry out these essential activities.