Ventral abdominal wall dysmorphogenesis of <i>Msx1/Msx2</i> double‐mutant mice

Ogi, Hidenao; Suzuki, Kentaro; Ogino, Yukiko; Kamimura, Mika; Miyado, Mami; Xu, Ying; Zhang, Zunyi; Shinohara, Masanori; Yamada, Gen

doi:10.1002/ar.a.20180

Cited by 29 publications

(33 citation statements)

References 48 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…It has thus been speculated that GT development requires correct adjacent tissue differentiation, such as lower body wall formation. Abnormal lower body wall formation associated with bladder/cloaca extrophy often simultaneously displays genital abnormalities such as the upper GT defects, and epispadias (Zhang et al, 1996;Brewer and Williams, 2004;Ogi et al, 2005;Haraguchi et al, unpublished results). In relation with such phenotypes, the presence or absence of cell migration between the umbilical region (later the lower body wall) and the (upper) GT bud requires further analyses.…”

Section: Appendage Phenotype Elicited By Aberrant Growth Factor Gene mentioning

confidence: 97%

Molecular genetic cascades for external genitalia formation: An emerging organogenesis program

Yamada

Suzuki

Haraguchi

et al. 2006

Developmental Dynamics

113

109

View full text Add to dashboard Cite

Section: Appendage Phenotype Elicited By Aberrant Growth Factor Gene mentioning

confidence: 97%

Molecular genetic cascades for external genitalia formation: An emerging organogenesis program

Yamada

Suzuki

Haraguchi

et al. 2006

Developmental Dynamics

113

109

View full text Add to dashboard Cite

“…AP-2␣ (Brewer and Williams, 2004a), Hoxb2/b4 double (Manley et al, 2001), Tgf␤2/␤3 double (Dunker and Krieglstein, 2002), and Mab21l2 (Yamada et al, 2004) mutants have defects in the primary body wall formation. The AP-2␣ mutant also lacks sternal and abdominal bands (Brewer and Williams, 2004a), and several mutants are known that have defects in the migration of the bands and/or in the subsequent clo-sure of the ventral body wall (Suzuki et al, 1996;Eggenschwiler et al, 1997;Zhang et al, 1997;Kitamura et al, 1999;Carter et al, 2000;Rauch et al, 2000;Doyonnas et al, 2001;Ogi et al, 2005;Thumkeo et al, 2005). However, the number of genes that participate in the ventral body wall formation is still too limited to discuss the molecular events of formation of this wall or pathologies of human defects.…”

Section: Introductionmentioning

confidence: 99%

A new serine/threonine protein kinase,Omphk1, essential to ventral body wall formation

Hirano¹,

Kanazawa

Furushima

et al. 2006

Developmental Dynamics

View full text Add to dashboard Cite

Here, we report a new serine/threonine protein kinase of the SNF1 subfamily Omphk1. Two Omphk homologues exist in each vertebrate species, and one homologue exists in Drosophila and Caenorhabditis elegans; the kinase domain is highly conserved among these homologues, and several domains are conserved among vertebrate Omphk. Omphk1 expression dynamically changes in the developing central nervous system, is found ubiquitously in epidermis, and is present uniquely in several other tissues. Its expression is also found in each tissue associated with the ventral body wall closure: the primary body wall composed of primitive ectoderm and each component of the secondary body wall. Concomitantly, its null mutant exhibits omphalocele with a failure in closure of the secondary body wall. There are no apparent gross morphological defects in brain, however, despite the unique Omphk1 expression in this tissue.

show abstract

“…Moreover, even at early stages, the complexity of the phenotype, the numerous embryological fields affected, and the interference between the defects elicited by the double mutation render the analysis difficult. For example, double mutants suffer from thoracoabdominoschisis (opening of both thorax and abdomen) (Ogi et al, 2005), which alters the development of all internal organs, and thus precludes the analysis of the role of Msx genes in these organs.…”

mentioning

confidence: 99%

Generation of an Msx2‐GFP conditional null allele

Bensoussan

Lallemand

Moreau

et al. 2008

Genesis

View full text Add to dashboard Cite

Msx1 and Msx2, two members of the Msx gene family, encode homeoprotein transcription factors and play critical roles during mouse development. Because of the redundancy between the two genes, many of these roles can only be studied in double Msx1; Msx2 mutants. However, these animals die around 14.5 dpc, which precludes analysis of Msx gene function beyond this stage. Moreover, the pleiotropic defects displayed by these embryos make phenotypic analysis difficult. To overcome these restrictions and study the double Msx mutant phenotype at later stages, we generated an Msx2 conditional null allele using Cre/loxP technology. The strategy consisted of flanking the Msx2 gene coding sequence with two loxP sites. In addition, a green fluorescent protein (GFP) reporter gene was placed under Msx2 regulatory sequences in the modified locus. Our results demonstrate that the Msx2-GFP conditional allele behaves as a normal one, whereas Cre-mediated recombination creates an Msx2 null allele. With either allele, expression patterns of the GFP reporter gene and the Msx2 endogenous gene are identical.

show abstract

Ventral abdominal wall dysmorphogenesis of Msx1/Msx2 double‐mutant mice

Cited by 29 publications

References 48 publications

Molecular genetic cascades for external genitalia formation: An emerging organogenesis program

Molecular genetic cascades for external genitalia formation: An emerging organogenesis program

A new serine/threonine protein kinase,Omphk1, essential to ventral body wall formation

Generation of an Msx2‐GFP conditional null allele

Contact Info

Product

Resources

About