Six1 and Six4 homeoproteins are required for Pax3 and Mrf expression during myogenesis in the mouse embryo

Author:

Grifone Raphaelle1,Demignon Josiane1,Houbron Christophe2,Souil Evelyne3,Niro Claire1,Seller Mary J.4,Hamard Ghislaine2,Maire Pascal1

Affiliation:

1. Département Génétique, Développement et Pathologie Moléculaire, Institut Cochin – INSERM 567, CNRS UMR 8104,Université Paris V, 24 Rue du Faubourg Saint Jacques 75014 Paris,France

2. Plateforme de recombinaison homologue, Institut Cochin – INSERM 567,CNRS UMR 8104, Université Paris V, 24 Rue du Faubourg Saint Jacques 75014 Paris, France

3. Plateforme d'histologie, Institut Cochin – INSERM 567, CNRS UMR 8104,Université Paris V, 24 Rue du Faubourg Saint Jacques 75014 Paris,France

4. Division of Medical and Molecular Genetics, Guy's Hospital, London SE1 9RT,UK

Abstract

In mammals, Six5, Six4 and Six1 genes are co-expressed during mouse myogenesis. Six4 and Six5 single knockout (KO)mice have no developmental defects, while Six1 KO mice die at birth and show multiple organ developmental defects. We have generated Six1Six4 double KO mice and show an aggravation of the phenotype previously reported for the single Six1 KO. Six1Six4 double KO mice are characterized by severe craniofacial and rib defects, and general muscle hypoplasia. At the limb bud level, Six1 and Six4homeogenes control early steps of myogenic cell delamination and migration from the somite through the control of Pax3 gene expression. Impaired in their migratory pathway, cells of the somitic ventrolateral dermomyotome are rerouted, lose their identity and die by apoptosis. At the interlimb level, epaxial Met expression is abolished, while it is preserved in Pax3-deficient embryos. Within the myotome, absence of Six1and Six4 impairs the expression of the myogenic regulatory factors myogenin and Myod1, and Mrf4 expression becomes undetectable. Myf5 expression is correctly initiated but becomes restricted to the caudal region of each somite. Early syndetomal expression of scleraxis is reduced in the Six1Six4 embryo, while the myotomal expression of Fgfr4 and Fgf8 but not Fgf4 and Fgf6 is maintained. These results highlight the different roles played by Six proteins during skeletal myogenesis.

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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