NeuroD-null mice are deaf due to a severe loss of the inner ear sensory neurons during development

W. Y. Kim; B. Fritzsch; A. Serls; L. A. Bakel; E. J. Huang; L. F. Reichardt; D. S. Barth; J. E. Lee

doi:10.1242/dev.128.3.417

NeuroD-null mice are deaf due to a severe loss of the inner ear sensory neurons during development

W. Y. Kim
, B. Fritzsch
, A. Serls
, L. A. Bakel
, E. J. Huang
, L. F. Reichardt
, D. S. Barth
, J. E. Lee

Research output: Contribution to journal › Article › peer-review

291 Scopus citations

Abstract

A key factor in the genetically programmed development of the nervous system is the death of massive numbers of neurons. Therefore, genetic mechanisms governing cell survival are of fundamental importance to developmental neuroscience. We report that inner ear sensory neurons are dependent on a basic helix-loop-helix transcription factor called NeuroD for survival during differentiation. Mice lacking NeuroD protein exhibit no auditory evoked potentials, reflecting a profound deafness. DiI fiber staining, immunostaining and cell death assays reveal that the deafness is due to the failure of inner ear sensory neuron survival during development. The affected inner ear sensory neurons fail to express neurotrophin receptors, TrkB and TrkC, suggesting that the ability of NeuroD to support neuronal survival may be directly mediated through regulation of responsiveness to the neurotrophins.

Original language	English
Pages (from-to)	417-426
Number of pages	10
Journal	Development
Volume	128
Issue number	3
DOIs	https://doi.org/10.1242/dev.128.3.417
State	Published - 2001

Keywords

Basic helix-loop-helix protein
Cell death
Deafness
Inner ear
Mouse
NeuroD
TrkB
TrkC

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10.1242/dev.128.3.417

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title = "NeuroD-null mice are deaf due to a severe loss of the inner ear sensory neurons during development",

abstract = "A key factor in the genetically programmed development of the nervous system is the death of massive numbers of neurons. Therefore, genetic mechanisms governing cell survival are of fundamental importance to developmental neuroscience. We report that inner ear sensory neurons are dependent on a basic helix-loop-helix transcription factor called NeuroD for survival during differentiation. Mice lacking NeuroD protein exhibit no auditory evoked potentials, reflecting a profound deafness. DiI fiber staining, immunostaining and cell death assays reveal that the deafness is due to the failure of inner ear sensory neuron survival during development. The affected inner ear sensory neurons fail to express neurotrophin receptors, TrkB and TrkC, suggesting that the ability of NeuroD to support neuronal survival may be directly mediated through regulation of responsiveness to the neurotrophins.",

keywords = "Basic helix-loop-helix protein, Cell death, Deafness, Inner ear, Mouse, NeuroD, TrkB, TrkC",

author = "Kim, \{W. Y.\} and B. Fritzsch and A. Serls and Bakel, \{L. A.\} and Huang, \{E. J.\} and Reichardt, \{L. F.\} and Barth, \{D. S.\} and Lee, \{J. E.\}",

year = "2001",

doi = "10.1242/dev.128.3.417",

language = "English",

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pages = "417--426",

journal = "Development",

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T1 - NeuroD-null mice are deaf due to a severe loss of the inner ear sensory neurons during development

AU - Kim, W. Y.

AU - Fritzsch, B.

AU - Serls, A.

AU - Bakel, L. A.

AU - Huang, E. J.

AU - Reichardt, L. F.

AU - Barth, D. S.

AU - Lee, J. E.

PY - 2001

Y1 - 2001

N2 - A key factor in the genetically programmed development of the nervous system is the death of massive numbers of neurons. Therefore, genetic mechanisms governing cell survival are of fundamental importance to developmental neuroscience. We report that inner ear sensory neurons are dependent on a basic helix-loop-helix transcription factor called NeuroD for survival during differentiation. Mice lacking NeuroD protein exhibit no auditory evoked potentials, reflecting a profound deafness. DiI fiber staining, immunostaining and cell death assays reveal that the deafness is due to the failure of inner ear sensory neuron survival during development. The affected inner ear sensory neurons fail to express neurotrophin receptors, TrkB and TrkC, suggesting that the ability of NeuroD to support neuronal survival may be directly mediated through regulation of responsiveness to the neurotrophins.

AB - A key factor in the genetically programmed development of the nervous system is the death of massive numbers of neurons. Therefore, genetic mechanisms governing cell survival are of fundamental importance to developmental neuroscience. We report that inner ear sensory neurons are dependent on a basic helix-loop-helix transcription factor called NeuroD for survival during differentiation. Mice lacking NeuroD protein exhibit no auditory evoked potentials, reflecting a profound deafness. DiI fiber staining, immunostaining and cell death assays reveal that the deafness is due to the failure of inner ear sensory neuron survival during development. The affected inner ear sensory neurons fail to express neurotrophin receptors, TrkB and TrkC, suggesting that the ability of NeuroD to support neuronal survival may be directly mediated through regulation of responsiveness to the neurotrophins.

KW - Basic helix-loop-helix protein

KW - Cell death

KW - Deafness

KW - Inner ear

KW - Mouse

KW - NeuroD

KW - TrkB

KW - TrkC

UR - https://www.scopus.com/pages/publications/0035123017

U2 - 10.1242/dev.128.3.417

DO - 10.1242/dev.128.3.417

M3 - Article

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AN - SCOPUS:0035123017

SN - 0950-1991

VL - 128

SP - 417

EP - 426

JO - Development

JF - Development

IS - 3

ER -

NeuroD-null mice are deaf due to a severe loss of the inner ear sensory neurons during development

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Keywords

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