AI Article Synopsis

  • S-SCAM is a synaptic protein that interacts with various components at inhibitory synapses, specifically beta-dystroglycan and neuroligin 2, indicating its crucial role in synapse structure and function.
  • The study shows that S-SCAM's WW domains bind to specific sequences in beta-DG, facilitating the formation of a tripartite complex with neuroligin 2, which is vital for inhibitory synaptic signaling.
  • Evidence of co-localization and interactions among S-SCAM, beta-DG, and neuroligin 2 suggests that S-SCAM acts as a connector linking the dystrophin glycoprotein complex with the neurexin-neuroligin complex at inhibitory

Article Abstract

Synaptic scaffolding molecule (S-SCAM) is a synaptic protein, which harbors five or six PSD-95/Discs large/ZO-1 (PDZ), a guanylate kinase and two WW domains. It interacts with NMDA receptor subunits, neuroligin and beta-catenin, and is involved in the accumulation of neuroligin at excitatory synapses. In this study, we have demonstrated S-SCAM is localized at inhibitory synapses in rat primary cultured hippocampal neurons. We have identified beta-dystroglycan (beta-DG) as a binding partner for S-SCAM at inhibitory synapses. WW domains of S-SCAM bind to three sequences of beta-DG. We have also revealed that S-SCAM can interact with neuroligin 2, which is known to be exclusively localized at inhibitory synapses. The WW domains and the second PDZ domain of S-SCAM are involved in the interaction with neuroligin 2. Beta-DG, neuroligin 2 and S-SCAM form a tripartite complex in vitro. Neuroligin 2 is detected in the immunoprecipitates by anti-beta-DG antibody from rat brain. S-SCAM, beta-DG and neuroligin 2 are partially co-localized in rat hippocampal neurons. These data suggest that S-SCAM is associated with beta-DG and neuroligin 2 at inhibitory synapses, and functions as a linker between the dystrophin glycoprotein complex and the neurexin-neuroligin complex.

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Source
http://dx.doi.org/10.1111/j.1471-4159.2006.04170.xDOI Listing

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