What makes a sodium channel?

The Rockefeller University Press $30.00 J. Gen. Physiol. 2016 Vol. 148 No. 2 89–90 www.jgp.org/cgi/doi/10.1085/jgp.201611652 89 Action potentials in mammalian nerve and muscle are carried by sodium currents through voltage-gated sodium channels (NaV). These proteins are part of the larger family of voltage-gated channels that includes the well-known calcium (CaV) and potassium (KV) channels, as well as a variety of other channel types, including Catsper, two-pore channels, and bacterial sodium channels (BacNaV). They even have distant homology to the IP3/ryanodine receptor, ionotropic glutamate receptor, and voltage-sensitive phosphatase families. However, it now seems that the large family of canonical NaV—the monophyletic group that includes all of the animal channels with typical Hodgkin-Huxley–like sodium currents—is a house divided: many appear to be selective for calcium. In this issue, GosselinBadaroudine et al. (2016. J. Gen. Physiol. http ://dx .doi .org /10 .1085 /jgp .201611614) describe a novel channel from the honeybee Apis mellifera that is the most calcium-selective NaV family member to date. One of the most interesting advances in recent years is that channels sharing the description “voltage gated” and “sodium channel” are not necessarily part of the same family, evolutionarily speaking. Instead, voltage-gated sodium channels seem to have evolved many times independently of one another, often within vastly different families of channels. These include bacterial channels that are only distantly related to eukaryotic NaVs (Ren et al., 2001; Liebeskind et al., 2013), intracellular two-pore channels (Wang et al., 2012), and even T-type CaVs (the latter being the result of a single splicing event; Senatore et al., 2014). One interesting observation is that many of these families have arisen from calcium channels (Liebeskind et al., 2012, 2013; Moran et al., 2015), confirming Hille’s assertion that canonical NaVs arose from CaVs (Hille, 1989) and extending it to other families. It seems that evolution has played the same trick time and time again, turning CaVs into NaVs. Even in the canonical NaV family, many members are likely to be calcium-selective channels (Zhou et al., 2004; Liebeskind et al., 2011; Gur Barzilai et al., 2012). Sodium selectivity within this family arose twice independently: once in vertebrates and once in cnidarians, such as jellyfish and sea anemones (Gur Barzilai et al., 2012). Thus, there exists a hidden world of channels that are phylogenetically NaV channels but biophysically CaV channels. These NaV/CaV channels have not been described until recently, perhaps because well-studied vertebrates have retained only the strictly NaV type (Liebeskind et al., 2011). Invertebrates, which form the vast majority of animal species, have kept the NaV/CaV type, and thus a major aspect of animal nervous systems, and a key part of our own history, has remained in the dark. In this issue, Gosselin-Badaroudine et al. provide the most thorough description of a NaV/CaV channel to date. Like others of its kind, the honeybee channel has a DEEA selectivity filter motif, intermediate, as it were, between the canonical NaV motif (DEKA) and the canonical CaV motifs (EEEE or EEDD). It also has much slower kinetics than the Hodgkin-Huxley–type NaV channels, operating on the scale of hundreds of milliseconds. The channel expresses robustly in Xenopus laevis oocytes, making it a prime candidate for a model NaV/CaV channel. But what makes this channel really interesting is that, unlike previously described NaV/CaV channels from cockroaches and sea anemones (Zhou et al., 2004; Gur Barzilai et al., 2012) that can pass both ions, it appears to have little or no sodium permeability. Sodium permeability was achieved by the authors after a single E→K mutation in the third domain, but even with this mutation, calcium still partially blocked conductance. Intriguingly, the block appeared to be insufficient to produce the anomalous mole fraction effect (AMFE) that typical CaV channels exhibit in mixed ionic solutions. This is an important difference. The classical view, put forward by Hille and others, is that sodium selectivity arose from calcium selectivity by removal of the high-affinity binding site for divalents, the site that gives rise to the AMFE in canonical calcium channels and allows them to “pluck rare calcium ions out of a sea of sodium” (Hille, 2001). Does the honeybee channel represent an intermediate state where the high-affinity site is partially removed? Does it represent a completely different mode of calcium selectivity? Does it select for the rare Ca ions without a high-affinity site? Or does it have a high-affinity site that, perhaps because of a unique pore geometry, does not give rise to an AMFE? This new channel raises a bevy What makes a sodium channel?