4.7 Article

Extracellular Signals Induce Glycoprotein M6a Clustering of Lipid Rafts and Associated Signaling Molecules

Journal

JOURNAL OF NEUROSCIENCE
Volume 37, Issue 15, Pages 4046-4064

Publisher

SOC NEUROSCIENCE
DOI: 10.1523/JNEUROSCI.3319-16.2017

Keywords

cholesterol; GPM6a; growth cone; lipid rafts; palmitoylation; polarity

Categories

Funding

  1. TOGONO Comprehensive Brain Science Network on Innovative Areas
  2. Niigata University
  3. Uehara Science Promoting Foundation
  4. RIKEN BioResource Center
  5. Tsukada Milk Company Research Grants
  6. KAKENHI from MEXT of Japan [17023019, 22240040, 24111515, 15K06770, 24700319]
  7. Grants-in-Aid for Scientific Research [15K06770, 16K07037, 24700319] Funding Source: KAKEN

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Lipid raft domains, where sphingolipids and cholesterol are enriched, concentrate signaling molecules. Toexaminehowsignaling protein complexes are clustered in rafts, we focused on the functions of glycoprotein M6a (GPM6a), which is expressed at a high concentration in developing mouse neurons. Using imaging of lipid rafts, we found that GPM6a congregated in rafts in a GPM6a palmitoylation-dependent manner, thereby contributing to lipid raft clustering. In addition, we found that signaling proteins downstream of GPM6a, such as Rufy3, Rap2, and Tiam2/STEF, accumulated in lipid rafts in a GPM6a-dependent manner and were essential for laminin-dependent polarity during neurite formation in neuronal development. In utero RNAi targeting of GPM6a resulted in abnormally polarized neurons with multiple neurites. These results demonstrate that GPM6a induces the clustering of lipid rafts, which supports the raft aggregation of its associated downstream molecules for acceleration of neuronal polarity determination. Therefore, GPM6a acts as a signal transducer that responds to extracellular signals.

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