| Literature DB >> 24012852 |
Juliane Dettling1, Christoph Franz1, Ulrike Zimmermann1, Sze Chim Lee1, Andreas Bress2, Niels Brandt3, Robert Feil4, Markus Pfister2, Jutta Engel3, Frédéric Flamant5, Lukas Rüttiger1, Marlies Knipper6.
Abstract
Thyroid hormone acts on gene transcription by binding to its nuclear receptors TRα1 and TRβ. Whereas global deletion of TRβ causes deafness, global TRα-deficient mice have normal hearing thresholds. Since the individual roles of the two receptors in cochlear hair cells are still unclear, we generated mice with a hair cell-specific mutation of TRα1 or deletion of TRβ using the Cre-loxP system. Hair cell-specific TRβ mutant mice showed normal hearing thresholds but delayed BK channel expression in inner hair cells, slightly stronger outer hair cell function, and slightly reduced amplitudes of auditory brainstem responses. In contrast, hair cell-specific TRα mutant mice showed normal timing of BK channel expression, slightly reduced outer hair cell function, and slightly enhanced amplitudes of auditory brainstem responses. Our data demonstrate that TRβ-related deafness originates outside of hair cells and that TRα and TRβ play opposing, non-redundant roles in hair cells. A role for thyroid hormone receptors in controlling key regulators that shape signal transduction during development is discussed. Thyroid hormone may act through different thyroid hormone receptor activities to permanently alter the sensitivity of auditory neurotransmission.Entities:
Keywords: ABR amplitudes; BK channel; Cochlear hair cells; Conditional mutant mice; Hypothyroidism; Thyroid hormone receptor α, β
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Year: 2013 PMID: 24012852 DOI: 10.1016/j.mce.2013.08.025
Source DB: PubMed Journal: Mol Cell Endocrinol ISSN: 0303-7207 Impact factor: 4.102