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Publication : Characterization of a novel thyroid hormone receptor alpha variant involved in the regulation of myoblast differentiation.

First Author  Casas F Year  2006
Journal  Mol Endocrinol Volume  20
Issue  4 Pages  749-63
PubMed ID  16322094 Mgi Jnum  J:107007
Mgi Id  MGI:3619869 Doi  10.1210/me.2005-0074
Citation  Casas F, et al. (2006) Characterization of a Novel Thyroid Hormone Receptor {alpha} Variant Involved in the Regulation of Myoblast Differentiation. Mol Endocrinol 20(4):749-63
abstractText  The regulation of gene expression by thyroid hormone (T(3)) involves binding of the hormone to nuclear receptors [thyroid hormone receptor (TR)] acting as T(3)-dependent transcription factors encoded by TRalpha (NR1A1) and TRbeta (NR1A2) genes. Several TRalpha variants have already been characterized, but only some of them display T(3) binding activity. In this study, we have identified another transcript, TRalpha-DeltaE6, produced by alternative splicing with microexon 6b instead of exon 6. This splicing leads to the synthesis of a protein devoid of a hinge domain. The TRalpha-DeltaE6 transcript is detected in all mouse tissues tested. Although TRalpha-DeltaE6 did not bind DNA, its expression induced a TRalpha1 sequestration in the cytoplasm. Functional studies demonstrated that TRalpha-DeltaE6 inhibits the transcriptional activity of TRalpha1 and retinoic X receptor-alpha, but not of retinoic acid receptor-alpha. We also found that TRalpha-DeltaE6 efficiently decreased the ability of TRalpha to inhibit MyoD transcriptional activity during myoblast proliferation. Consequently, when overexpressed in myoblasts, it stimulated terminal differentiation. We suggest that this novel TRalpha variant may act as down regulator of overall T(3) receptor activity, including its ability to repress MyoD transcriptional activity during myoblast proliferation.
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