The forkhead/winged-helix gene, Mf1, is necessary for the normal development of the cornea and formation of the anterior chamber in the mouse eye

Susan H. Kidson*, Tsutomu Kume, Keyu Deng, Virginia Winfrey, Brigid L M Hogan

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

151 Scopus citations

Abstract

Mf1, which encodes a winged-helix/forkhead transcription factor, is the murine homolog of human FKHL7, mutated in individuals with autosomal dominant inherited dysgenesis of the anterior segment of the eye (Axenfeld-Reiger anomaly). Mouse embryos homozygous for null mutations in Mf1 (Mf1(lacZ) and Mf1(ch)) show severely abnormal development of the anterior segment. The cornea fails to separate from the lens, resulting in the complete absence of an anterior chamber. There is no differentiation of the inner corneal endothelial layer, as judged by electron microscopy and by absence of labeling with monoclonal antibody to zonula occludens protein 1, a normal component of occluding junctions in wild-type endothelial cells. In addition, the mutant corneal stroma is disorganized and the epithelium thicker than normal. The Mf1 gene is normally expressed in the periocular mesenchyme at E11.5 but is downregulated as the corneal endothelium differentiates. In contrast, Mf1(lacZ) expression persists longer in mutant corneal mesenchyme, and abnormal expression is also seen in the mutant corneal epithelium. Based on classical studies with the chick embryonic eye, a model is proposed for the differentiation of the mammalian corneal endothelium from mesenchyme in response to putative signals from the lens. Possible roles for Mf1 in this process are discussed.

Original languageEnglish (US)
Pages (from-to)306-322
Number of pages17
JournalDevelopmental Biology
Volume211
Issue number2
DOIs
StatePublished - Jul 15 1999

Funding

We thank Drs. Simon John and Richard Smith, The Jackson Laboratory, for many helpful and stimulating discussions and Dr. Jenny Narraway, The Hubrecht Laboratory, for help in the loan of slides. We also thank Drs. Peter Dempsey and Maureen Gannon and members of the Hogan Laboratory, Vanderbilt Medical Center, for advice and critical comments on the manuscript. Confocal microscopy was carried out in the VUMC Cell Imaging Resource Center (supported by CA 68485 and DK 20593). T.K. is an Associate and B.L.M.H. an Investigator of the Howard Hughes Medical Institute. S.H.K. was supported by sabbatical travel grants from the Medical Research Councils of South Africa and the University of Cape Town.

Keywords

  • Cornea
  • Endothelium
  • Eye development
  • Forkhead winged helix gene
  • Mf1/FKHL7
  • Mouse embryo
  • Mutant
  • Zonula occludens protein 1

ASJC Scopus subject areas

  • Molecular Biology
  • Cell Biology
  • Developmental Biology

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