Genetic interaction between Lef1 and Alx4 is required for early embryonic development

Genetic interaction between Lef1 and Alx4 is required for early embryonic development

Lymphoid Enhancer Factor-1 (Lef1) facilitates the assembly of transcriptional regulatory complexes and mediates nuclear responses to Wnt signals. We determined previously that the mesenchymally restricted, paired-like homeodomain protein Aristaless-like 4 (Alx4) interacts with Lef1 and together alte...

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Bibliographic Details
Published in:The International journal of developmental biology Vol. 50; no. 7; pp. 601 - 610
Main Authors: Boras-Granic, Kata, Grosschedl, Rudolf, Hamel, Paul A
Format: Journal Article
Language:English
Published: Spain 2006
Subjects:
Animals
Crosses, Genetic
Embryonic Development
Female
Fluorescent Antibody Technique, Direct
Gene Expression Regulation, Developmental
Heterozygote
Homeodomain Proteins - genetics
Homeodomain Proteins - metabolism
Immunohistochemistry
Lymphoid Enhancer-Binding Factor 1 - genetics
Lymphoid Enhancer-Binding Factor 1 - metabolism
Mice
Mice, Inbred C57BL
Mice, Knockout
Neovascularization, Pathologic - embryology
Platelet Endothelial Cell Adhesion Molecule-1 - metabolism
Pregnancy
Yolk Sac - blood supply
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Summary:Lymphoid Enhancer Factor-1 (Lef1) facilitates the assembly of transcriptional regulatory complexes and mediates nuclear responses to Wnt signals. We determined previously that the mesenchymally restricted, paired-like homeodomain protein Aristaless-like 4 (Alx4) interacts with Lef1 and together alters promoter activity of candidate genes. In order to define their overlapping functions, mice deficient for both Lef1 and Alx4 activity (Lef1-/-/Alx4lstD/lstD) were produced. Whereas embryos lacking either Lef1 or Alx4 activity remain viable up to or after birth, early embryonic lethality results when both factors were absent. No viable Lef1-/-/Alx4lstD/lstD embryos were recovered beyond 9.5 dpc. Between E8.5 and E10, viable Lef1-/-/Alx4lstD/lstD embryos were developmentally delayed 0.5 days relative to littermates of all other genotypes. Principle among the alterations seen in Lef1-/-/Alx4lstD/lstD animals was defective vasculature in both embryonic and extra-embryonic tissues. In the yolk sac, while the vascular network is present, it were greatly diminished and large vitelline vessels were largely absent. Platelet/endothelial cell adhesion molecule (PECAM) staining revealed that the major vessels in the head of compound mutant embryos were absent, while the other vessels were finer than those seen in normal littermates. Pools of blood and pericardial effusion were also apparent in Lef1-/-/Alx4lstD/lstD animals, further indicative of a defective vasculature. These data confirm genetically the interaction between Lef1 and Alx4 and further reveal unknown, overlapping roles for these transcription factors in embryonic vasculogenesis.
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ISSN:0214-6282
DOI:10.1387/ijdb.062153kb