In response to injury, skeletal muscle exhibits high capacity to regenerate and epigenetics controls multiple steps of this process (Giordani et al., 2013). It has been demonstrated in vitro that completion of muscle differentiation requires shuttling of histone deacetylase 4 (HDAC4), a member of class IIa HDACs, from the nucleus to the cytoplasm and consequent activation of MEF2-dependent differentiation genes (McKinsey et al., 2000). In vivo, HDAC4 expression is up-regulated in skeletal muscle upon injury, suggesting a role for this protein in muscle regeneratio

ADAMO, Sergio

C. Noviello

E. N. Olson

MARRONCELLI, NICOLETTA

MORESI, Viviana

P. L. Puri

S. Consalvi

V. Saccone

English

In response to injury, skeletal muscle exhibits high capacity to regenerate and epigenetics controls multiple steps of this process (Giordani et al., 2013). It has been demonstrated in vitro that completion of muscle differentiation requires shuttling of histone deacetylase 4 (HDAC4), a member of class IIa HDACs, from the nucleus to the cytoplasm and consequent activation of MEF2-dependent differentiation genes (McKinsey et al., 2000). In vivo, HDAC4 expression is up-regulated in skeletal muscle upon injury, suggesting a role for this protein in muscle regeneration. With the aim to elucidate the role of HDAC4 in skeletal muscle regeneration, we generate mice lacking HDAC4 in the satellite cells (HDAC4fl/fl;Pax7CE Cre). Lack of HDAC4 inhibits satellite cell differentiation. Despite having similar amount of sorted cells, HDAC4 KO satellite cells proliferate less and have less pax7 than controls. Importantly, muscle regeneration in vivo is impaired in HDAC4fl/fl;Pax7CE Cre mice. These results are confirmed by molecular analyses of the expression of myogenic markers. All together, these data delineate the importance of HDAC4 in muscle regeneration and suggest a protective role in response to muscle damage

Marroncelli, Nicoletta

Noviello, Chiara

Consalvi, Silvia

Saccone, Valentina

Puri, Pier Lorenzo

Olson, Eric N.

Adamo, Sergio

Moresi, Viviana

Firenze University Press: E-Journals

IJAE 
Vo l .  119,  n .  1  (Supp lem ent) :  126 ,  2014
© 2014 Firenze University Press 
ht tp://www.fupress .com/ijae
ITALIAN JOURNAL OF ANATOMY AND EMBRYOLOGY
HDAC4 is necessary for satellite cell differentiation and 
muscle regeneration
Nicoletta Marroncelli1, Chiara 1, Silvia Consalvi2, Valentina Saccone2, Pier Lorenzo Puri2, Eric N. 
Olson3, Sergio Adamo1, Viviana Moresi1
1 Dept. of Anat., Histol., Forens. & Orthop. Sciences, Sapienza University of Rome, Italy
2 Istituto di Ricovero e Cura a Carattere Scientifico (IRCCS) Fondazione Santa Lucia, 00143 Rome, Italy
3 Dept. of Molecular Biology, University of Texas Southwestern Medical Center, Dallas, TX, USA
In response to injury, skeletal muscle exhibits high capacity to regenerate and 
epigenetics controls multiple steps of this process (Giordani et al., 2013). It has been 
demonstrated in vitro that completion of muscle differentiation requires shuttling of 
histone deacetylase 4 (HDAC4), a member of class IIa HDACs, from the nucleus to 
the cytoplasm and consequent activation of MEF2-dependent differentiation genes 
(McKinsey et al., 2000). In vivo, HDAC4 expression is up-regulated in skeletal mus-
cle upon injury, suggesting a role for this protein in muscle regeneration. With the 
aim to elucidate the role of HDAC4 in skeletal muscle regeneration, we generate mice 
lacking HDAC4 in the satellite cells (HDAC4fl/fl;Pax7CE Cre). Lack of HDAC4 inhib-
its satellite cell differentiation. Despite having similar amount of sorted cells, HDAC4 
KO satellite cells proliferate less and have less pax7 than controls. Importantly, mus-
cle regeneration in vivo is impaired in HDAC4fl/fl;Pax7CE Cre mice. These results are 
confirmed by molecular analyses of the expression of myogenic markers. All together, 
these data delineate the importance of HDAC4 in muscle regeneration and suggest a 
protective role in response to muscle damage.
References
Giordani L, Puri PL. Epigenetic control of skeletal muscle regeneration: Integrating genetic determi-
nants and environmental changes. FEBS J. 2013 Sep;280(17):4014-25.
McKinsey TA, Zhang CL, Lu J, Olson EN. Signal-dependent nuclear export of a histone deacetylase 
regulates muscle differentiation. Nature. 2000 Nov 2;408(6808):106-11.
Keywords
Histone acetylation, chromatin remodeling, transcriptional regulation of gene expression, satel-
lite cell commitment, muscle repair.


HDAC4 is necessary for satellite cell differentiation and muscle regeneration

Modulation of specific gene response following physiological and pathological signaling require multiple levels of transcriptional control. In response to injury, skeletal muscle exhibits high capacity to regenerate and epigenetics controls multiple steps of this process. In vitro has been demonstrated that completion of muscle differentiation requires shuttling of histone deacetylase 4 (HDAC4), a member of class IIa HDACs, from the nucleus to the cytoplasm and consequent activation of MEF2-dependent differentiation genes

Archivio della ricerca- Università di Roma La Sapienza

In response to injury, skeletal muscle exhibits high capacity to regenerate and epigenetics controls multiple steps of this process. In vitro has been demonstrated that completion of muscle differentiation requires shuttling of histone deacetylase 4 (HDAC4), a member of class IIa HDACs, from the nucleus to the cytoplasm and consequent activation of MEF2-dependent differentiation genes. In vivo, HDAC4 expression is up-regulated in skeletal muscle upon injury, suggesting a role for this protein in muscle regeneration. With the aim to elucidate the role of HDAC4 in skeletal muscle regeneration, we generate mice lacking HDAC4 in the satellite cells (HDAC4fl/fl;Pax7CE Cre). Lack of HDAC4 inhibits satellite cell differentiation. Despite having similar amount of sorted cells, HDAC4 KO satellite cells proliferate less and have less pax7 than controls. Importantly, muscle regeneration in vivo is impaired in HDAC4fl/fl;Pax7CE Cre mice. These results are confirmed by molecular analyses of the expression of myogenic markers. All together, these data delineate the importance of HDAC4 in muscle regeneration and suggest a protective role in response to muscle damag

LXVIII Convegno SIAI – Ancona 2014 - It J Anat Embryol 119: 2014  HDAC4 is necessary for satellite cell differentiation and muscle regeneration. Nicoletta Marroncellia, Chiara Novielloa, Silvia Consalvib, Valentina Sacconeb, Pier Lorenzo Purib, Eric N. Olsonc, Sergio Adamoa and Viviana Moresia. a Dept. of Anat., Histol., Forens. & Orthop. Sciences, Sapienza University of Rome, Italy b Istituto di Ricovero e Cura a Carattere Scientifico (IRCCS) Fondazione Santa Lucia, 00143 Rome, Italy c Dept. of Molecular Biology, University of Texas Southwestern Medical Center, Dallas, TX, USA In response to injury, skeletal muscle exhibits high capacity to regenerate and epigenetics controls multiple steps of this process (Giordani et al., 2013). It has been demonstrated in vitro that completion of muscle differentiation requires shuttling of histone deacetylase 4 (HDAC4), a member of class IIa HDACs, from the nucleus to the cytoplasm and consequent activation of MEF2-dependent differentiation genes (McKinsey et al., 2000). In vivo, HDAC4 expression is up-regulated in skeletal muscle upon injury, suggesting a role for this protein in muscle regeneration. With the aim to elucidate the role of HDAC4 in skeletal muscle regeneration, we generate mice lacking HDAC4 in the satellite cells (HDAC4fl/fl;Pax7CE Cre). Lack of HDAC4 inhibits satellite cell differentiation. Despite having similar amount of sorted cells, HDAC4 KO satellite cells proliferate less and have less pax7 than controls. Importantly, muscle regeneration in vivo is impaired in HDAC4fl/fl;Pax7CE Cre mice. These results are confirmed by molecular analyses of the expression of myogenic markers. All together, these data delineate the importance of HDAC4 in muscle regeneration and suggest a protective role in response to muscle damage. References (1) Giordani L, Puri PL. Epigenetic control of skeletal muscle regeneration: Integrating genetic determinants and environmental changes. FEBS J. 2013 Sep;280(17):4014-25. (2) McKinsey TA, Zhang CL, Lu J, Olson EN. Signal-dependent nuclear export of a histone deacetylase regulates muscle differentiation. Nature. 2000 Nov 2;408(6808):106-11.  Keywords Histone acetylation, chromatin remodeling, transcriptional regulation of gene expression, satellite cell commitment, muscle repair.   

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HDAC4 is necessary for satellite cell differentiation and muscle regeneration

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