Literature DB >> 18585463

Multiple cell adhesion molecules shaping a complex nicotinic synapse on neurons.

Gallen B Triana-Baltzer1, Zhaoping Liu, Natalia V Gounko, Darwin K Berg.   

Abstract

Neuroligin, SynCAM, and L1-CAM are cell adhesion molecules with synaptogenic roles in glutamatergic pathways. We show here that SynCAM is expressed in the chick ciliary ganglion, embedded in a nicotinic pathway, and, as shown previously for neuroligin and L1-CAM, acts transcellularly to promote synaptic maturation on the neurons in culture. Moreover, we show that electroporation of chick embryos with dominant negative constructs disrupting any of the three molecules in vivo reduces the total amount of presynaptic SV2 overlaying the neurons expressing the constructs. Only disruption of L1-CAM and neuroligin, however, reduces the number of SV2 puncta specifically overlaying nicotinic receptor clusters. Disrupting L1-CAM and neuroligin together produces no additional decrement, indicating that they act on the same subset of synapses. SynCAM may affect synaptic maturation rather than synapse formation. The results indicate that individual neurons can express multiple synaptogenic molecules with different effects on the same class of nicotinic synapses.

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Year:  2008        PMID: 18585463      PMCID: PMC2600484          DOI: 10.1016/j.mcn.2008.05.017

Source DB:  PubMed          Journal:  Mol Cell Neurosci        ISSN: 1044-7431            Impact factor:   4.314


  47 in total

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Authors:  William G Conroy; Zhaoping Liu; Qiang Nai; Jay S Coggan; Darwin K Berg
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  10 in total

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Review 2.  Postsynaptic scaffolds for nicotinic receptors on neurons.

Authors:  Robert A Neff; David Gomez-Varela; Catarina C Fernandes; Darwin K Berg
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6.  Synchronous and asynchronous transmitter release at nicotinic synapses are differentially regulated by postsynaptic PSD-95 proteins.

Authors:  Robert A Neff; William G Conroy; Jeffrey D Schoellerman; Darwin K Berg
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8.  Identification of gene transcripts expressed by postsynaptic neurons during synapse formation encoding cell surface proteins with presumptive synaptogenic activity.

Authors:  Juan L Brusés
Journal:  Synapse       Date:  2010-01       Impact factor: 2.562

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  10 in total

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