| Literature DB >> 26491026 |
Ke Liu1, Fei Ji1, Guan Yang2, Zhaohui Hou1, Jianhe Sun1, Xiaoyu Wang1, Weiwei Guo1, Wei Sun3, Weiyan Yang1, Xiao Yang4, Shiming Yang5.
Abstract
More than 100 genes have been associated with deafness. However, SMAD4 is rarely considered a contributor to deafness in humans, except for its well-defined role in cell differentiation and regeneration. Here, we report that a SMAD4 defect in mice can cause auditory neuropathy, which was defined as a mysterious hearing and speech perception disorder in human for which the genetic background remains unclear. Our study showed that a SMAD4 defect induces failed formation of cochlear ribbon synapse during the earlier stage of auditory development in mice. Further investigation found that there are nearly normal morphology of outer hair cells (OHCs) and post-synapse spiral ganglion nerves (SGNs) in SMAD4 conditional knockout mice (cKO); however, a preserved distortion product of otoacoustic emission (DPOAE) and cochlear microphonic (CM) still can be evoked in cKO mice. Moreover, a partial restoration of hearing detected by electric auditory brainstem response (eABR) has been obtained in the cKO mice using electrode stimuli toward auditory nerves. Additionally, the ribbon synapses in retina are not affected by this SMAD4 defect. Thus, our findings suggest that this SMAD4 defect causes auditory neuropathy via specialized disruption of cochlear ribbon synapses.Entities:
Keywords: Auditory neuropathy; Cochlea; Deafness; Retina; Ribbon synapse; SMAD4
Mesh:
Substances:
Year: 2015 PMID: 26491026 DOI: 10.1007/s12035-015-9454-1
Source DB: PubMed Journal: Mol Neurobiol ISSN: 0893-7648 Impact factor: 5.590