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RNA steady-state defects in myotonic dystrophy are linked to nuclear exclusion of SHARP.


ABSTRACT: We describe a new mechanism by which CTG tract expansion affects myotonic dystrophy (DM1). Changes to the levels of a panel of RNAs involved in muscle development and function that are downregulated in DM1 are due to aberrant localization of the transcription factor SHARP (SMART/HDAC1-associated repressor protein). Mislocalization of SHARP in DM1 is consistent with increased CRM1-mediated export of SHARP to the cytoplasm. A direct link between CTG repeat expression and SHARP mislocalization is demonstrated as expression of expanded CTG repeats in normal cells recapitulates cytoplasmic SHARP localization. These results demonstrate a role for the inactivation of SHARP transcription in DM1 biology.

SUBMITTER: Dansithong W 

PROVIDER: S-EPMC3128970 | biostudies-literature | 2011 Jul

REPOSITORIES: biostudies-literature

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RNA steady-state defects in myotonic dystrophy are linked to nuclear exclusion of SHARP.

Dansithong Warunee W   Jog Sonali P SP   Paul Sharan S   Mohammadzadeh Robabeh R   Tring Stephanie S   Kwok Yukwah Y   Fry Rebecca C RC   Marjoram Paul P   Comai Lucio L   Reddy Sita S  

EMBO reports 20110701 7


We describe a new mechanism by which CTG tract expansion affects myotonic dystrophy (DM1). Changes to the levels of a panel of RNAs involved in muscle development and function that are downregulated in DM1 are due to aberrant localization of the transcription factor SHARP (SMART/HDAC1-associated repressor protein). Mislocalization of SHARP in DM1 is consistent with increased CRM1-mediated export of SHARP to the cytoplasm. A direct link between CTG repeat expression and SHARP mislocalization is d  ...[more]

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