• Neuroscience · Mar 2008

    Schwann cells genetically modified to express neurotrophins promote spiral ganglion neuron survival in vitro.

    • L N Pettingill, R L Minter, and R K Shepherd.
    • The Bionic Ear Institute, 384 Albert Street, East Melbourne, Australia 3002. lpettingill@bionicear.org
    • Neuroscience. 2008 Mar 27; 152 (3): 821-8.

    AbstractThe intracochlear infusion of neurotrophic factors via a mini-osmotic pump has been shown to prevent deafness-induced spiral ganglion neuron (SGN) degeneration; however, the use of pumps may increase the incidence of infection within the cochlea, making this technique unsuitable for neurotrophin administration in a clinical setting. Cell- and gene-based therapies are potential therapeutic options. This study investigated whether Schwann cells which were genetically modified to over-express the neurotrophins brain-derived neurotrophic factor (BDNF) or neurotrophin 3 (Ntf3, formerly NT-3) could support SGN survival in an in vitro model of deafness. Co-culture of either BDNF over-expressing Schwann cells or Ntf3 over-expressing Schwann cells with SGNs from early postnatal rats significantly enhanced neuronal survival in comparison to both control Schwann cells and conventional recombinant neurotrophin proteins. Transplantation of neurotrophin over-expressing Schwann cells into the cochlea may provide an alternative means of delivering neurotrophic factors to the deaf cochlea for therapeutic purposes.

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