L1CAM binds ErbB receptors through Ig-like domains coupling cell adhesion and neuregulin signalling.

PLoS One

Instituto de Neurociencias de Alicante, Universidad Miguel Hernández-Spanish National Research Council, San Juan de Alicante, Spain.

Published: March 2013

AI Article Synopsis

  • The development of the nervous system involves various cell-to-cell communication methods that help neurons and axons navigate and form complex networks, but the coordination of these processes is not well understood.
  • Cross-regulatory interactions and redundancy in signaling pathways can enhance the precision of these guidance systems.
  • L1CAM, an immunoglobulin superfamily protein, physically interacts with erbB receptors, which boosts their responsiveness to neuregulins during neuron development and may help target specific cells or axons that engage with L1CAM.

Article Abstract

During nervous system development different cell-to-cell communication mechanisms operate in parallel guiding migrating neurons and growing axons to generate complex arrays of neural circuits. How such a system works in coordination is not well understood. Cross-regulatory interactions between different signalling pathways and redundancy between them can increase precision and fidelity of guidance systems. Immunoglobulin superfamily proteins of the NCAM and L1 families couple specific substrate recognition and cell adhesion with the activation of receptor tyrosine kinases. Thus it has been shown that L1CAM-mediated cell adhesion promotes the activation of the EGFR (erbB1) from Drosophila to humans. Here we explore the specificity of the molecular interaction between L1CAM and the erbB receptor family. We show that L1CAM binds physically erbB receptors in both heterologous systems and the mammalian developing brain. Different Ig-like domains located in the extracellular part of L1CAM can support this interaction. Interestingly, binding of L1CAM to erbB enhances its response to neuregulins. During development this may synergize with the activation of erbB receptors through L1CAM homophilic interactions, conferring diffusible neuregulins specificity for cells or axons that interact with the substrate through L1CAM.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3398014PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0040674PLOS

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