Title : MDGAs interact selectively with neuroligin-2 but not other neuroligins to regulate inhibitory synapse development - Lee_2013_Proc.Natl.Acad.Sci.U.S.A_110_336 |
Author(s) : Lee K , Kim Y , Lee SJ , Qiang Y , Lee D , Lee HW , Kim H , Je HS , Sudhof TC , Ko J |
Ref : Proc Natl Acad Sci U S A , 110 :336 , 2013 |
Abstract :
The MAM domain-containing GPI anchor proteins MDGA1 and MDGA2 are Ig superfamily adhesion molecules composed of six IG domains, a fibronectin III domain, a MAM domain, and a GPI anchor. MDGAs contribute to the radial migration and positioning of a subset of cortical neurons during early neural development. However, MDGAs continue to be expressed in postnatal brain, and their functions during postnatal neural development remain unknown. Here, we demonstrate that MDGAs specifically and with a nanomolar affinity bind to neuroligin-2, a cell-adhesion molecule of inhibitory synapses, but do not bind detectably to neuroligin-1 or neuroligin-3. We observed no cell adhesion between cells expressing neuroligin-2 and MDGA1, suggesting a cis interaction. Importantly, RNAi-mediated knockdown of MDGAs increased the abundance of inhibitory but not excitatory synapses in a neuroligin-2-dependent manner. Conversely, overexpression of MDGA1 decreased the numbers of functional inhibitory synapses. Likewise, coexpression of both MDGA1 and neuroligin-2 reduced the synaptogenic capacity of neuroligin-2 in an artificial synapse-formation assay by abolishing the ability of neuroligin-2 to form an adhesion complex with neurexins. Taken together, our data suggest that MDGAs inhibit the activity of neuroligin-2 in controlling the function of inhibitory synapses and that MDGAs do so by binding to neuroligin-2. |
PubMedSearch : Lee_2013_Proc.Natl.Acad.Sci.U.S.A_110_336 |
PubMedID: 23248271 |
Lee K, Kim Y, Lee SJ, Qiang Y, Lee D, Lee HW, Kim H, Je HS, Sudhof TC, Ko J (2013)
MDGAs interact selectively with neuroligin-2 but not other neuroligins to regulate inhibitory synapse development
Proc Natl Acad Sci U S A
110 :336
Lee K, Kim Y, Lee SJ, Qiang Y, Lee D, Lee HW, Kim H, Je HS, Sudhof TC, Ko J (2013)
Proc Natl Acad Sci U S A
110 :336