Abstract
Targets of neuronal innervations play a vital role in regulating the survival and differentiation of innervating neurotrophin-responsive neurons. During development, neurons extend axons to their targets, and then their survival become dependent on the trophic substances secreted by their target cells. Sensory endings were present on myoblasts, myotubes, and myofibers in all intrafusal bundles regardless of age. The interdependence of sensory neurons and skeletal muscle (SKM) cells during both embryonic development and the maintenance of the mature functional state has not been fully understood. In the present study, neuromuscular cocultures of organotypic dorsal root ganglion (DRG) explants and dissociate SKM cells were established. Using this culture system, the morphological relationship between DRG neurons and SKM cells, neurites growth and neuronal migration were investigated. The migrating neurons were determined by fluorescent labeling of microtubule-associated protein-2 (MAP-2) and neurofilament 200 (NF-200) or growth-associated protein 43 (GAP-43). The expression of NF-200 and GAP-43 and their mRNAs was evaluated by Western blot assay and real time-PCR analysis. The results reveal that DRG explants showed more dense neurites outgrowth in neuromuscular cocultures as compared with that in the culture of DRG explants alone. The number of total migrating neurons (the MAP-2-expressing neurons) and the percentage NF-200-immunoreactive (IR) and GAP-43-IR neurons increased significantly in the presence of SKM cells. The levels of NF-200 and GAP-43 and their mRNAs increased significantly in neuromuscular cocultures as compared with that in the culture of DRG explants alone. These results suggested that target SKM cells play an important role in regulating neuronal protein synthesis, promoting neuritis outgrowth and neuronal migration of DRG explants in vitro. These results not only provide new clues for a better understanding of the association of SKM cells with DRG sensory neurons during development, they may also have implications for axonal regeneration after nerve injury.
Highlights
Targets of neuronal innervations play a vital role in regulation of the survival and differentiation of innervating neurotrophin (NT)-responsive neurons [1]
We investigated the contribution of target tissues to neuronal outgrowth, migration and expression of neurofilament 200 (NF-200) and growth-associated protein 43 (GAP-43)
Some axons terminate upon contact with the contracting skeletal muscle (SKM) cells, others may choose to ignore the surfaces of SKM cells
Summary
Targets of neuronal innervations play a vital role in regulation of the survival and differentiation of innervating neurotrophin (NT)-responsive neurons [1]. The motor neurons and skeletal muscle (SKM) fibers innervations depend on each other strongly [2,3]. Important communication between both tissues is mediated through the neuromuscular junction. NTs potentiate presynaptic release of neurotransmitter [5,6] and are essential for motor neuron survival [7], as well as for the maintenance of postsynaptic characteristic develop and maturation of muscle. Synapse-forming axons have vital effect on cell-surface behavior at nerve-muscle contacts during synaptogenesis in co-cultures of rat ventral spinal cord neurons and myotubes [8]. Innervations induce formation of a mature SKM-like excitation-contraction coupling system in cultured human muscle cells [10]. Sensory nerve cross-anastomosis (sensory protection) provides a modified trophic environment by modulating neurotrophic factor synthesis in muscle [14]
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