Moreover, there is abundant evidence demonstrating that sodium channels participate in or regulate
multiple effector functions in these nonexcitable cells. It is becoming clear, for example, that sodium channels—located not only on the plasma membrane delimiting the cell from the extracellular Epigenetic inhibitor library space but also, in some cases, on intracellular membranes surrounding specific organelles within the cell—contribute to processes as diverse as phagocytosis, motility, the release of bioactive molecules, and the regulation of Na+/K+-ATPase activity in nonneuronal cells, including cells as disparate as microglia and astrocytes within the CNS, where they participate in the response to CNS injury, and cancer cells, where they contribute to motility and invasiveness. The neuroscience community, which has a long history of discoveries on sodium channels and their function and which possesses an armamentarium of powerful tools that can help explicate the function of
sodium Alisertib channels, is in a unique position to elucidate the functions of sodium channels in nonexcitable cells, as well as in neurons. In this article, we discuss the expression of sodium channels in nonexcitable cells and review accumulating evidence showing that, within these cells, these channels play noncanonical roles and participate in multiple, diverse effector functions. It is now known that nine different genes encode nine distinct sodium channels (Nav1.1–Nav1.9),
which are expressed with diverse temporal and regional patterns in excitable cells (Catterall et al., 2005) and are variably associated with β-subunits (Patino and Isom, 2010 and Brackenbury and Isom, 2011). Although all voltage-gated sodium channels share a common overall structural motif and considerable homology, the different subtypes display distinct voltage dependence and kinetic and pharmacological properties (Catterall et al., 2005), Rutecarpine and the repertoire of sodium channel subtypes expressed in a particular type of excitable cell significantly contributes to its pattern of electroresponsiveness (see, e.g., Waxman, 2000 and Rush et al., 2007). Nav1.1, Nav1.2, and Nav1.6 are expressed in both central and peripheral neurons, whereas Nav1.7–Nav1.9 are preferentially expressed in peripheral neurons (Beckh et al., 1989, Felts et al., 1997, Gong et al., 1999, Schaller and Caldwell, 2003, Catterall et al., 2005 and Dib-Hajj et al., 2013). Nav1.3 is present in the adult human brain (Chen et al., 2000, Whitaker et al., 2001 and Thimmapaya et al., 2005), but it is predominantly expressed during embryonic and early postnatal periods in rodents. Nav1.3 is upregulated in dorsal root ganglion neurons in adult rodents after nerve injury (Waxman et al.