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      Specific features of neuronal size and shape are regulated by tropomyosin isoforms.

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          Abstract

          Spatially distinct populations of microfilaments, characterized by different tropomyosin (Tm) isoforms, are present within a neuron. To investigate the impact of altered tropomyosin isoform expression on neuronal morphogenesis, embryonic cortical neurons from transgenic mice expressing the isoforms Tm3 and Tm5NM1, under the control of the beta-actin promoter, were cultured in vitro. Exogenously expressed Tm isoforms sorted to different subcellular compartments with Tm5NM1 enriched in filopodia and growth cones, whereas the Tm3 was more broadly localized. The Tm5NM1 neurons displayed significantly enlarged growth cones accompanied by an increase in the number of dendrites and axonal branching. In contrast, Tm3 neurons displayed inhibition of neurite outgrowth. Recruitment of Tm5a and myosin IIB was observed in the peripheral region of a significant number of Tm5NM1 growth cones. We propose that enrichment of myosin IIB increases filament stability, leading to the enlarged growth cones. Our observations support a role for different tropomyosin isoforms in regulating interactions with myosin and thereby regulating morphology in specific intracellular compartments.

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          Author and article information

          Journal
          Mol Biol Cell
          Molecular biology of the cell
          American Society for Cell Biology (ASCB)
          1059-1524
          1059-1524
          Jul 2005
          : 16
          : 7
          Affiliations
          [1 ] Oncology Research Unit, The Children's Hospital at Westmead, Westmead NSW 2145, Australia.
          Article
          E04-10-0951
          10.1091/mbc.e04-10-0951
          1165423
          15888546
          7d3633f8-c057-421d-a94f-450b3b3bd01d
          History

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