AI Article Synopsis

  • The plasma membrane of growth cones in axons is constantly changing during navigation and target recognition.
  • Researchers discovered a new bulk endocytic pathway that plays a key role in membrane recycling, particularly at sites with high actin activity.
  • During early development, this bulk endocytosis is crucial for membrane retrieval, but as synapses begin to form, it decreases, allowing for more specific synaptic processes to take over.

Article Abstract

The growth-cone plasma membrane constantly reconfigures during axon navigation and upon target recognition. The identity and regulation of the membrane pathway(s) participating in remodeling of the growth-cone surface remain elusive. Here, we identify a constitutive, high-capacity plasma-membrane-recycling activity in the axonal growth cones, which is mediated by a novel bulk endocytic pathway that is mechanistically related to macropinocytosis. This pathway generates large compartments at sites of intense actin-based membrane ruffling through the actions of phosphatidylinositol 3-kinase, the small GTPase Rac1 and the pinocytic chaperone Pincher. At early developmental stages, bulk endocytosis is the primary endocytic pathway for rapid retrieval of the growth-cone plasma membrane. At later stages, during the onset of synaptogenesis, an intrinsic program of maturation leads to downregulation of basal bulk endocytosis and the emergence of depolarization-induced synaptic-vesicle exo-endocytosis. We propose that the control of bulk membrane retrieval contributes to the homeostatic regulation of the axonal plasma membrane and to growth-cone remodeling during axonal outgrowth. In addition, we suggest that the downregulation of bulk endocytosis during synaptogenesis might contribute to the preservation of synaptic-vesicle specificity.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2731302PMC
http://dx.doi.org/10.1242/jcs.033803DOI Listing

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