Abstract

This proposal will investigate gene transfer and cell death in the cochlea. Gene transfer has recently become an important method for tissue engineering for experimental and clinical purposes. The experimental field of inner ear biology and the otology clinic may benefit greatly from gene transfer technology. Viral vectors have become the vehicle of choice for in vivo genetic interventions in the nervous system. The cochlea may be among the organs that can benefit from genetic manipulation via viral vectors. We have demonstrated efficient infection of guinea pig spiral ganglion cells in vitro and in vivo with the Ad.RSVntlacZ adenoviral vector. Transgene expression has been detected as long as eight weeks after the inoculation. In this application we propose to continue our successful preliminary experiments to optimize variable parameters of adenoviral mediated gene transfer into cochlear cells. Specifically, we will (a) determine the optimal inoculation parameters needed for efficient infection of spiral ganglion cells, (b) characterize the immune response to the viral infection, (c) determine the duration of viral gene expression, (d) characterize the spread of infection to adjacent tissues, and (e) determine the functionality of infected spiral ganglion cells using ABR measurements. We also propose to determine the effects of gene transfer on spiral ganglion cell survival. Specifically, we will determine if it is possible to (a) rescue spiral ganglion cells by overexpressing bcl-2 and (b) induce cell death in spiral ganglion cells by viral-mediated overexpression of bcl-xs. The data we have been generating, along with the experiments we now propose will solidify the foundation of viral mediated gene transfer in the cochlea. This technology will facilitate experimental elimination of specific cell types in the cochlea, and create a powerful tool for physiological studies in this organ. As such, it will be of benefit to the other projects described in our Program Project. Moreover, gene transfer will enable to study function of specific genes in the ear. It will also help the important clinical goal of preserving spiral ganglion cells, for reducing progressive trauma and enhancing benefits from cochlear implants.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Deafness and Other Communication Disorders (NIDCD)
Type
Research Program Projects (P01)
Project #
2P01DC000078-32A2
Application #
6270070
Study Section
Project Start
1997-12-01
Project End
1998-11-30
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
32
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Type
DUNS #
791277940
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Stefanescu, Roxana A; Koehler, Seth D; Shore, Susan E (2015) Stimulus-timing-dependent modifications of rate-level functions in animals with and without tinnitus. J Neurophysiol 113:956-70
Basura, Gregory J; Koehler, Seth D; Shore, Susan E (2015) Bimodal stimulus timing-dependent plasticity in primary auditory cortex is altered after noise exposure with and without tinnitus. J Neurophysiol 114:3064-75
Le Prell, Colleen G; Hughes, Larry F; Bledsoe Jr, Sanford C (2014) Dynorphin release by the lateral olivocochlear efferents may inhibit auditory nerve activity: a cochlear drug delivery study. Neurosci Lett 571:17-22
Le Prell, Colleen G; Dolan, David F; Hughes, Larry F et al. (2014) Disruption of lateral olivocochlear neurons with a dopaminergic neurotoxin depresses spontaneous auditory nerve activity. Neurosci Lett 582:54-8
Koehler, Seth D; Shore, Susan E (2013) Stimulus-timing dependent multisensory plasticity in the guinea pig dorsal cochlear nucleus. PLoS One 8:e59828
Basura, Gregory J; Koehler, Seth D; Shore, Susan E (2012) Multi-sensory integration in brainstem and auditory cortex. Brain Res 1485:95-107
Dehmel, Susanne; Pradhan, Shashwati; Koehler, Seth et al. (2012) Noise overexposure alters long-term somatosensory-auditory processing in the dorsal cochlear nucleus--possible basis for tinnitus-related hyperactivity? J Neurosci 32:1660-71
Koehler, Seth D; Pradhan, Shashwati; Manis, Paul B et al. (2011) Somatosensory inputs modify auditory spike timing in dorsal cochlear nucleus principal cells. Eur J Neurosci 33:409-20
Bledsoe Jr, Sanford C; Koehler, Seth; Tucci, Debara L et al. (2009) Ventral cochlear nucleus responses to contralateral sound are mediated by commissural and olivocochlear pathways. J Neurophysiol 102:886-900
Skjonsberg, Asa; Halsey, Karin; Ulfendahl, Mats et al. (2007) Exploring efferent-mediated DPOAE adaptation in three different guinea pig strains. Hear Res 224:27-33

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