REGENERATIVE PHENOMENA IN THE DEVELOPING ORGAN OF CORTI
Project Number5R01DC000844-02
Contact PI/Project LeaderSOBKOWICZ, HANNA M
Awardee OrganizationUNIVERSITY OF WISCONSIN-MADISON
Description
Abstract Text
The long-term goal of the proposed research is to gain understanding of
the process of regeneration of sensory and nerve cells following
mechanical injury to the cochlea in culture, and to define the factors
that lead to their morphological recovery. In light of the lack of overt
evidence proving that the mammalian organ of Corti is able to form new
sensory cells, and given the fact that these cells are few and may be
formed only once in a life span the significance of the research lies in
understanding the mechanism of survival and recovery of receptor cells
after injury.
Specifically, we propose to study: 1) Post-traumatic cell proliferation
in the organ of Corti: A) Mitotic cell proliferation in the injured
cultures will be examined using 3H thymidine to investigate the identity
of dividing cells, the duration of the mitotic response and the age-
related occurrence of cell division; B) Nonmitotic cell proliferation,
expressed by extensive sprouting of supporting cells, will be
investigated in search of possible diffusable growth factors (NGF, EGF,
FGF) released by the cells in response to direct injury or to the injury
of sensory cells. 2) Regeneration of the injured sensory cells,
especially the reformation of their cuticular plates and stereocilia.
The study will encompass the morphological sequence of the regenerative
phenomena, its comparison with normal development, and the influence of
age on the regenerative capacity of sensory cells. 3) Degeneration and
regeneration of spiral neurons, sprouting of their endings (using
antibodies to GAP-43 and NF proteins), and formation of new ribbon
synapses.
The study will be done using short- and long-term cultures of the mouse
organ of Corti. The injury will be done by hand, using either a pulled-
glass pipettes or a laser. Light and electron microscopy,
autoradiography, biochemistry and immunocytochemistry will be employed.
Some specialized immunological assays will be done in collaboration with
Dr. Philippe Lefebvre, University de Liege, Belgium.
Public Health Relevance Statement
Data not available.
NIH Spending Category
No NIH Spending Category available.
Project Terms
cell cycledevelopmental neurobiologyear hair cellelectron microscopyepidermal growth factorfibroblast growth factorimmunocytochemistryinjurylaboratory mousenervous system regenerationneural degenerationneurotrophic factorsnewborn animalsorgan of Cortisynaptogenesistissue /cell culture
National Institute on Deafness and Other Communication Disorders
CFDA Code
DUNS Number
161202122
UEI
LCLSJAGTNZQ7
Project Start Date
01-July-1992
Project End Date
30-June-1996
Budget Start Date
01-July-1993
Budget End Date
30-June-1994
Project Funding Information for 1993
Total Funding
$167,792
Direct Costs
$122,633
Indirect Costs
$45,159
Year
Funding IC
FY Total Cost by IC
1993
National Institute on Deafness and Other Communication Disorders
$167,792
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 5R01DC000844-02
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