Boc modifies the holoprosencephaly spectrum of Cdo mutant mice

Dis Model Mech. 2011 May;4(3):368-80. doi: 10.1242/dmm.005744. Epub 2010 Dec 23.

Abstract

Holoprosencephaly (HPE) is caused by a failure to form the midline of the forebrain and/or midface. It is one of the most common human birth defects, but clinical expression is extremely variable. HPE is associated with mutations in the sonic hedgehog (SHH) pathway. Mice lacking the Shh pathway regulator Cdo (also called Cdon) display HPE with strain-dependent penetrance and expressivity, implicating silent modifier genes as one cause of the variability. However, the identities of potential HPE modifiers of this type are unknown. We report here that whereas mice lacking the Cdo paralog Boc do not have HPE, Cdo;Boc double mutants on a largely Cdo-resistant genetic background have lobar HPE with strong craniofacial anomalies and defects in Shh target gene expression in the developing forebrain. Boc is therefore a silent HPE modifier gene in mice. Furthermore, Cdo and Boc have specific, selective roles in Shh signaling in mammals, because Cdo;Boc double-mutant mice do not display the most severe HPE phenotype seen in Shh-null mice, nor do they have major defects in digit patterning or development of vertebrae, which are also Shh-dependent processes. This is in contrast to reported observations in Drosophila, where genetic removal of the Cdo and Boc orthologs Ihog and Boi results in a complete loss of response to the hedgehog ligand. Therefore, there is evolutionary divergence between mammals and insects in the requirement of the hedgehog pathway for Cdo/Ihog family members, with mammalian development involving additional factors and/or distinct mechanisms at this level of pathway regulation.

Publication types

  • Research Support, N.I.H., Extramural
  • Research Support, Non-U.S. Gov't

MeSH terms

  • Animals
  • Bone Development
  • Cell Adhesion Molecules / deficiency*
  • Cell Adhesion Molecules / genetics
  • Cell Adhesion Molecules / metabolism
  • Embryo, Mammalian / abnormalities
  • Embryo, Mammalian / metabolism
  • Embryo, Mammalian / pathology
  • Extremities / embryology
  • Fibroblast Growth Factor 8 / genetics
  • Fibroblast Growth Factor 8 / metabolism
  • Gene Expression Regulation, Developmental
  • Hedgehog Proteins / genetics
  • Hedgehog Proteins / metabolism
  • Holoprosencephaly / metabolism*
  • Holoprosencephaly / pathology*
  • Humans
  • Immunoglobulin G / genetics
  • Immunoglobulin G / metabolism*
  • Mice
  • Mice, Mutant Strains
  • Palate / embryology
  • Palate / metabolism
  • Palate / pathology
  • Phenotype
  • Polymerase Chain Reaction
  • Prosencephalon / embryology
  • Prosencephalon / metabolism
  • Prosencephalon / pathology
  • Receptors, Cell Surface / deficiency
  • Receptors, Cell Surface / genetics
  • Receptors, Cell Surface / metabolism*
  • Signal Transduction
  • Species Specificity

Substances

  • Boc protein, mouse
  • Cdon protein, mouse
  • Cell Adhesion Molecules
  • Fgf8 protein, mouse
  • Hedgehog Proteins
  • Immunoglobulin G
  • Receptors, Cell Surface
  • Shh protein, mouse
  • Fibroblast Growth Factor 8