, 2004). Disruption of collybistin in mice leads to increased levels of anxiety and impaired spatial learning, which are associated with a selective loss of GABAARs in the hippocampus and basolateral amygdala (Papadopoulos et al., 2007). In humans, a missense mutation in the collybistin SH3 domain results in somatic and dendritic trapping of gephyrin and inhibitory Selleckchem Pritelivir receptors by collybistin aggregates, giving rise to a hyperekplexia, drug-resistant seizures and premature death (Harvey et al., 2004). Collybistin that has been activated by NL2 associates with the

postsynaptic plasma membrane and promotes the subsynaptic clustering of gephyrin. This has led to the conclusion that complexes of NL2, collybistin and gephyrin are sufficient to generate the clustering of postsynaptic GABAARs, even in the absence of a presynaptic terminal (Poulopoulos et al., 2009). Whether, or for how long, such a structure would be stable remains to be determined. It has also been proposed that the interplay between neurexins and neuroligins is modified to maintain the balance between the excitation and inhibition that a neurone receives. Shifts in the location of NL1 and NL2 to excitatory synapses are associated with overexpression of PSD-95 and an increase in the ratio of excitatory

to inhibitory synaptic Olaparib solubility dmso currents; a decrease in this ratio follows knock-down of PSD-95 (Prange et al., 2004; Levinson et al., 2005; Levinson & El Husseini, 2005, for review). There are many other cell adhesion molecules, some of which are found in the synaptic cleft. Some of these are selectively expressed at glutamatergic synapses, e.g. SynCAM (synaptic cell adhesion molecules), ephrins (ligands of class V-EPH-related – receptor

protein-tyrosine kinases), ephrin receptors and netrin-G ligands (transmembrane protein Org 27569 ligands of secreted proteins that act as long-range cues for growth cones). Others, such as NCAM (neural cell adhesion molecule), localise to GABAergic synapses and promote their formation and/or stabilisation (Pillai-Nair et al., 2005). Postsynaptically derived dystroglycan accumulates at a subset of mature GABAergic synapses, but only after the formation and aggregation of presynaptic vesicles and the clustering of postsynaptic GABAARs, particularly of α2-subunit-containing GABAARs (Lévi et al., 2002). β-Dystroglycan is a binding partner for S-SCAM (synaptic scaffolding molecule) at inhibitory synapses, forming a tripartite complex with NL2 in vitro, with S-SCAM acting as a link between NL2 and β-dystroglycan (Sumita et al., 2007). α-Neurexins also bind dystroglycan, but only via LNS2 and LNS6 domains that lack splice inserts (Sugita et al., 2001). Craig & Kang (2007) suggest that cell adhesion molecules may initiate interactions between putative pre- and postsynaptic elements and that neurexin–neuroligin interactions then recruit and stabilise other pre- and postsynaptic structures.