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Anatomical, Metabolic and genetic aspects of age-related hearing loss in mice

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65 Scopus citations

Abstract

Because of their short lifespan and genetic homogeneity, mice can provide valuable insights into the biological basis of age-related hearing loss. In C57BL/6 mice, hair cell loss begins around 1–2 months of age and progresses rapidly along a base-to-apex gradient, whereas CBA mice show relatively little hair cell loss until late in life. This anatomical difference is reflected in dehydrogenase histochemistry, an indirect measure of aerobic energy metabolism. A small, but significant, decrease in hair cell dehydrogenase staining occurred in CBA mice between 1.5 and 18 months of age. Significantly, dehydrogenase levels in 1.5-month C57 mice were substantially lower than in CBA mice of any age. Thus, deficits in aerobic energy metabolism presage degeneration of the hair cells. The superoxide radical, O 2 , a normal byproduct of cellular metabolism, is potentially toxic and can cause cellular damage if it is not inactivated by superoxide dismutases. Cytosolic copper/zinc superoxide dismutase (SOD 1) is highly expressed in the cochlea. Knockout mutant mice with a single (HET) or double deletion (KO) of the Sodl gene coding for SOD1 showed greater age-related losses than wild-type (WT) mice. KO mice had the worst hearing, WT the best, and HETs were intermediate. KOs exhibited considerably greater hair cell loss than WT mice; however, losses in KOs were only slightly greater than in HETs. KO mice showed significantly greater loss of spiral ganglion cells and nerve fibers than WT mice. These results indicate that SOD1 and O 2 play important roles in age-related hearing loss. Intervention strategies targeting O 2 may reduce age-related hearing loss.

Original languageEnglish
Pages (from-to)313-321
Number of pages9
JournalInternational Journal of Audiology
Volume40
Issue number6
DOIs
StatePublished - 2001

Keywords

  • C57
  • CBA
  • Dehydrogenase
  • Glycogen
  • Hair cells
  • Knockout mice
  • Presbyacusis
  • Spiral ganglion
  • Stria vascularis
  • Superoxide dismutase

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