HES6 is a novel member of the family of basic helix–loop–helix mammalian homologues of Drosophila Hairy and Enhancer of split. We have analyzed the biochemical and functional roles of HES6 in myoblasts. HES6 interacted with the corepressor transducin-like Enhancer of split 1 in yeast and mammalian cells through its WRPW COOH-terminal motif. HES6 repressed transcription from an N box–containing template and also when tethered to DNA through the GAL4 DNA binding domain. On N box–containing promoters, HES6 cooperated with HES1 to achieve maximal repression. An HES6–VP16 activation domain fusion protein activated the N box–containing reporter, confirming that HES6 bound the N box in muscle cells. The expression of HES6 was induced when myoblasts fused to become differentiated myotubes. Constitutive expression of HES6 in myoblasts inhibited expression of MyoR, a repressor of myogenesis, and induced differentiation, as evidenced by fusion into myotubes and expression of the muscle marker myosin heavy chain. Reciprocally, blocking endogenous HES6 function by using a WRPW-deleted dominant negative HES6 mutant led to increased expression of MyoR and completely blocked the muscle development program. Our results show that HES6 is an important regulator of myogenesis and suggest that MyoR is a target for HES6-dependent transcriptional repression.
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17 September 2001
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September 10 2001
HES6 acts as a transcriptional repressor in myoblasts and can induce the myogenic differentiation program
Xiangming Gao,
Xiangming Gao
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
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Tanya Chandra,
Tanya Chandra
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
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Michel-Olivier Gratton,
Michel-Olivier Gratton
2Center for Neuronal Survival, Montreal Neurological Institute, Montréal, Québec, Canada H3A 2B4
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Isabelle Quélo,
Isabelle Quélo
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
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Josée Prud'homme,
Josée Prud'homme
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
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Stefano Stifani,
Stefano Stifani
2Center for Neuronal Survival, Montreal Neurological Institute, Montréal, Québec, Canada H3A 2B4
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René St-Arnaud
René St-Arnaud
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
3Departments of Surgery and Human Genetics, McGill University, Montréal H3A 2T5, Québec, Canada
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Xiangming Gao
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
Tanya Chandra
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
Michel-Olivier Gratton
2Center for Neuronal Survival, Montreal Neurological Institute, Montréal, Québec, Canada H3A 2B4
Isabelle Quélo
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
Josée Prud'homme
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
Stefano Stifani
2Center for Neuronal Survival, Montreal Neurological Institute, Montréal, Québec, Canada H3A 2B4
René St-Arnaud
1Genetics Unit, Shriners Hospital for Children, Montréal H3G 1A6, Québec, Canada
3Departments of Surgery and Human Genetics, McGill University, Montréal H3A 2T5, Québec, Canada
Address correspondence to René St-Arnaud, Genetics Unit, Shriners Hospital for Children, 1529 Cedar Ave., Montréal H3G 1A6, Québec, Canada. Tel.: (514) 282-7155. Fax: (514) 842-5581. E-mail: [email protected]
*
Abbreviations used in this paper: bHLH, basic domain helix–loop–helix; DM, differentiation medium; GM, growth medium; GST, glutathione S-transferase; MHC, myosin heavy chain; MyoR, myogenic repressor; RT, reverse transcriptase; TLE, transducin-like Enhancer of split; TPR, tetratricopeptide repeat.
Received:
April 13 2001
Revision Received:
August 02 2001
Accepted:
August 06 2001
Online ISSN: 1540-8140
Print ISSN: 0021-9525
The Rockefeller University Press
2001
J Cell Biol (2001) 154 (6): 1161–1172.
Article history
Received:
April 13 2001
Revision Received:
August 02 2001
Accepted:
August 06 2001
Citation
Xiangming Gao, Tanya Chandra, Michel-Olivier Gratton, Isabelle Quélo, Josée Prud'homme, Stefano Stifani, René St-Arnaud; HES6 acts as a transcriptional repressor in myoblasts and can induce the myogenic differentiation program . J Cell Biol 17 September 2001; 154 (6): 1161–1172. doi: https://doi.org/10.1083/jcb.200104058
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