Molecular Characterization of Axon-Glial Interactions
Our work demonstrates the presence of axo-glial septate junctions (AGSJs) inDrosophila nerves and establishes structural and molecular similarities betweenDrosophila and vertebrate AGSJs. Drosophila proteins: Neurexin IV (NRX IV), Contactin(CONT) and Neuroglian (NRG) form a tripartite complex that localizes to AGSJs. Theirmurine orthologs Contactin-associated protein (Caspr), Contactin (Cont) andNeurofascin (NF155) also form a complex at the paranodal AGSJs in myelinated axons.Drosophila nrx IV, cont and nrg, and mouse Caspr, Cont and NF155 mutants all fail toorganize AGSJs. In addition, double mutant combinations and triple mutants of nrx IV,cont and nrg in Drosophila show severe peripheral glial migration defects and axonaldegeneration in embryonic peripheral nerves, pointing to an important relationshipbetween axon-glial interactions and axonal/glial cytoskeleton. We also discovered thatin the embryonic CNS midline NRX IV functions independent of CONT and NRG, andinteracts in trans with a midline glia-specific immunoglobulin (Ig) domain protein,Wrapper (WRAP). This interaction coordinates axon-glial interactions, axonalensheathment and glial migration in the CNS midline. Together these studies lead us tohypothesize that glial migration, ensheathment, and axon degeneration aremechanistically linked. Our findings provide the basis to approach the fundamentalquestion of how axonal ensheathment is coordinated with underlying axonal and glialcytoskeletal elements during neuron-glial interactions. Most importantly, we ask whichaxon-glial signaling mechanisms are essential for maintaining axonal health andneuronal functions. Identification of these mechanisms using in vivo genetic analysis willprovide a basis for our attempts to identify the cellular and molecular mechanismsprecipitating pathological demyelination and impeding remyelination. PUBLIC HEALTH RELEVANCE: Molecular Characterization of Axon-Glial Interactions The studies described in this renewal grant application relate to the genetic and molecular mechanisms that govern axonal ensheathment, establishment of neuro-glial scaffolds and organization of specialized electron-dense structures, the axo-glial septate junctions (AGSJs). This unique structure coordinates axonal domains and allows myelinated axons to propagate nerve impulses in a saltatory manner. Better understanding of the fundamental mechanisms that underlie axonal ensheathment and organization of axonal domains will help in designing future therapeutic strategies to myelin-related diseases or demyelination disorders like for example multiple sclerosis (MS) where remyelination is required and the axonal domain structure must be preserved to allow action potential propagation.