TNF Inhibition of Skeletal Muscle Regeneration is Mediated by a Caspase Dependent Stem Cell Response

doi:10.1634/stemcells.2007-0493

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First published online February 7, 2008
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Submitted on June 21, 2007
Accepted on January 15, 2008

TISSUE-SPECIFIC STEM CELLS

TNF Inhibition of Skeletal Muscle Regeneration is Mediated by a Caspase Dependent Stem Cell Response

Viviana Moresi ¹, Alessandro Pristerà ¹, Bianca M. Scicchitano ¹, Mario Molinaro ¹, Laura Teodori ¹, David Sassoon ², Sergio Adamo ¹^*, Dario Coletti ¹

¹ Department of Histology and Medical Embryology and Interuniversity Institute of Myology, Sapienza University, Rome, ITALY; Myology Group Inserm U787, Université Pierre et Marie Curie-Paris 6, UMR S, Paris, FRANCE, 75013
² Biotechmed, ENEA-Casaccia, Rome, ITALY; Myology Group Inserm U787, Université Pierre et Marie Curie-Paris 6, UMR S, Paris, FRANCE, 75013

^* To whom correspondence should be addressed. E-mail: sergio.adamo{at}uniroma1.it.

Abstract

Skeletal muscle is susceptible to injury following trauma,neurological dysfunction, and genetic diseases. Skeletal musclehomeostasis is maintained by a pronounced regenerative capacitywhich includes the recruitment of stem cells. Chronic exposureto tumor necrosis factor-alpha (TNF) triggers a muscle wastingreminiscent of cachexia. To better understand the effects ofTNF upon muscle homeostasis and stem cells, we exposed injuredmuscle to TNF at specific time-points during regeneration. TNFexposure delayed the appearance of regenerating fibers, withoutexacerbating fiber death following the initial trauma. We observedmodest cellular caspase activation during regeneration whichis markedly increased in response to TNF exposure concomitantwith an inhibition in regeneration. Caspase activation did notlead to apoptosis and did not involve caspase-3. Inhibitionof caspase activity improved muscle regeneration either in theabsence or presence of TNF, revealing a non apoptotic role forthis pathway in the myogenic program. Caspase activity was localizedto the interstitial cells which also express Sca1, CD34 andPW1. Perturbation of PW1 activity blocked caspase activationand improved regeneration. The restricted localization of Sca1⁺,CD34⁺, PW1⁺ cells to a subset of interstitial cells with caspaseactivity reveals a critical regulatory role for this populationduring myogenesis, which may directly contribute to residentmuscle stem cells or indirectly regulate stem cells throughcell-cell interactions.

Key Words. Peg3/PW1, adult stem cells, muscle stem cells, cytokines, caspase assay, gene delivery by electroporation

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