Functional and morphological recovery of dystrophic muscles in mice treated with deacetylase inhibitors
GC Minetti, C Colussi, R Adami, C Serra, C Mozzetta… - Nature medicine, 2006 - nature.com
GC Minetti, C Colussi, R Adami, C Serra, C Mozzetta, V Parente, S Fortuni, S Straino…
Nature medicine, 2006•nature.comPharmacological interventions that increase myofiber size counter the functional decline of
dystrophic muscles,. We show that deacetylase inhibitors increase the size of myofibers in
dystrophin-deficient (MDX) and α-sarcoglycan (α-SG)–deficient mice by inducing the
expression of the myostatin antagonist follistatin in satellite cells. Deacetylase inhibitor
treatment conferred on dystrophic muscles resistance to contraction-coupled degeneration
and alleviated both morphological and functional consequences of the primary genetic …
dystrophic muscles,. We show that deacetylase inhibitors increase the size of myofibers in
dystrophin-deficient (MDX) and α-sarcoglycan (α-SG)–deficient mice by inducing the
expression of the myostatin antagonist follistatin in satellite cells. Deacetylase inhibitor
treatment conferred on dystrophic muscles resistance to contraction-coupled degeneration
and alleviated both morphological and functional consequences of the primary genetic …
Abstract
Pharmacological interventions that increase myofiber size counter the functional decline of dystrophic muscles,. We show that deacetylase inhibitors increase the size of myofibers in dystrophin-deficient (MDX) and α-sarcoglycan (α-SG)–deficient mice by inducing the expression of the myostatin antagonist follistatin in satellite cells. Deacetylase inhibitor treatment conferred on dystrophic muscles resistance to contraction-coupled degeneration and alleviated both morphological and functional consequences of the primary genetic defect. These results provide a rationale for using deacetylase inhibitors in the pharmacological therapy of muscular dystrophies.
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