There are five types of kainate receptor subunits,
GluR5 (),
GluR6 (),
GluR7 (),
KA1 () and
KA2 (), which are similar to AMPA and NMDA receptor subunits and can be arranged in different ways to form a
tetramer, a four subunit receptor. GluR5-7 can form homomers (ex. a receptor composed entirely of GluR5) and heteromers (ex. a receptor composed of both GluR5 and GluR6), however, KA1 and KA2 can only form functional receptors by combining with one of the GluR5-7 subunits. Since 2009 the kainate receptor subunits have been renamed to correspond with their gene name. Hence GluR5-7 are now GluK1-3 and KA1 and KA2 are GluK4 and GluK5, respectively. Each KAR subunit begins with a 400-residue extracellular N-terminal domain, which plays a key role in assembly, followed by the first segment of the neurotransmitter-binding cleft, called S1. This segment then passes through the
cell membrane, forming the first of three membrane-spanning regions, M1. The M2 segment then begins on the
cytoplasmic face of the membrane, pushes into the
cell membrane about halfway, and then dips back out to the cytoplasm. This segment, termed the "p loop," determines the calcium permeability of the receptor. M2 turns into M3, another transmembrane segment which emerges on the extracellular face to complete the neurotransmitter binding site (a portion called S2). M4 begins extracellularly, and passes again through the membrane into the cytoplasm, forming the C-terminal of the protein. Differences in the ligand binding pocket allow for the development of moderately subunit-selective kainate receptor agonists and antagonists. ==Conductance==