Gene profiling of skeletal muscle in an amyotrophic lateral sclerosis mouse model

doi:10.1152/physiolgenomics.00017.2007

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Physiol. Genomics 32: 207-218, 2008. First published November 13, 2007; doi:10.1152/physiolgenomics.00017.2007
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Received 16 January 2007; accepted in final form 12 November 2007.
Physiological Genomics 32:207-218 (2008)
1094-8341/08 $8.00 © 2008 American Physiological Society

Gene profiling of skeletal muscle in an amyotrophic lateral sclerosis mouse model

Jose-Luis Gonzalez de Aguilar ¹^,2, Christa Niederhauser-Wiederkehr ³, Benoît Halter ¹^,2, Marc De Tapia ¹^,2, Franck Di Scala ¹^,2, Philippe Demougin ³, Luc Dupuis ¹^,2, Michael Primig ³, Vincent Meininger ⁴ and Jean-Philippe Loeffler ¹^,2

¹ Institut National de la Santé et de la Recherche Médicale, U692, Laboratoire de Signalisations Moléculaires et Neurodégénérescence, Strasbourg
² Université Louis Pasteur, Faculté de Médecine, Unité Mixte de Recherche en Santé-692, Strasbourg, France
³ Biozentrum and Swiss Institute of Bioinformatics, Basel, Switzerland
⁴ Hôpital de la Pitié-Salpêtrière, Fédération des Maladies du Système Nerveux, Centre Référent Maladie Rare Sclérose Latérale Amyotrophique, Paris, France

Muscle atrophy is a major hallmark of amyotrophic lateral sclerosis(ALS), the most frequent adult-onset motor neuron disease. Todefine the full set of alterations in gene expression in skeletalmuscle during the course of the disease, we used the G86R superoxidedismutase-1 transgenic mouse model of ALS and performed high-densityoligonucleotide microarrays. We compared these data to thoseobtained by axotomy-induced denervation. A major set of generegulations in G86R muscles resembled those of surgically denervatedmuscles, but many others appeared specific to the ALS condition.The first significant transcriptional changes appeared in asubpopulation of mice before the onset of overt clinical symptomsand motor neuron death. These early changes affected genes involvedin detoxification (e.g., ALDH3, metallothionein-2, and thioredoxin-1)and regeneration (e.g., BTG1, RB1, and RUNX1) but also tissuedegradation (e.g., C/EBP ${delta}$ and DDIT4) and cell death (e.g., ankyrinrepeat domain-1, CDKN1A, GADD45 ${alpha}$ , and PEG3). Of particular interest,metallothionein-1 and -2, ATF3, cathepsin-Z, and galectin-3genes appeared, among others, commonly regulated in both skeletalmuscle (our present data) and spinal motor neurons (as previouslyreported) of paralyzed ALS mice. The importance of these findingsis twofold. First, they designate the distal part of the motorunit as a primary site of disease. Second, they identify specificgene regulations to be explored in the search for therapeuticstrategies that could alleviate disease before motor neurondeath manifests clinically.

atrophy; axotomy; denervation; neuromuscular disease