APA
Modamio Høybjør, Silvia & Mencía, Ángeles & Goodyear, Richard & del Castillo, Ignacio & Richardson, Guy & Moreno, Felipe & Moreno Pelayo, Miguel Ángel (2007-06 ) .A Mutation in CCDC50, a Gene Encoding an Effector of Epidermal Growth Factor¿Mediated Cell Signaling, Causes Progressive Hearing Loss.
ISO 690
Modamio Høybjør, Silvia & Mencía, Ángeles & Goodyear, Richard & del Castillo, Ignacio & Richardson, Guy & Moreno, Felipe & Moreno Pelayo, Miguel Ángel. 2007-06 .A Mutation in CCDC50, a Gene Encoding an Effector of Epidermal Growth Factor¿Mediated Cell Signaling, Causes Progressive Hearing Loss.
https://hdl.handle.net/20.500.12080/39717
Resumen:
We previously mapped a novel autosomal dominant deafness locus, DFNA44, by studying a family with postlingual,
progressive, nonsyndromic hearing loss. We report here on the identification of a mutation in CCDC50 as the cause of
hearing loss in the family. CCDC50 encodes Ymer, an effector of epidermal growth factor (EGF)¿mediated cell signaling
that is ubiquitously expressed in different organs and has been suggested to inhibit down-regulation of the EGF receptor.
We have examined its expression pattern in mouse inner ear. Western blotting and cell transfection results indicate that
Ymer is a soluble, cytoplasmic protein, and immunostaining shows that Ymer is expressed in a complex spatiotemporal
pattern during inner ear development. In adult inner ear, the expression of Ymer is restricted to the pillar cells of the
cochlea, the stria vascularis, and the vestibular sensory epithelia, where it shows spatial overlap with the microtubule based cytoskeleton. In dividing cells, Ymer colocalizes with microtubules of the mitotic apparatus. We suggest that DFNA44
hearing loss may result from a time-dependent disorganization of the microtubule-based cytoskeleton in the pillar cells
and stria vascularis of the adult auditory system.