The Hemimelic extra toes mouse mutant: Historical perspective on unraveling mechanisms of dysmorphogenesis

Hemimelic extra toes (Hx) arose spontaneously as a dominant mutation in B10.D2/nSnJ mice in 1967. It specifically affects the appendicular skeleton, causing variable foreshortening of the tibia (radius) and preaxial polydactylism. Early anatomical studies revealed anterior overgrowth of the autopod,...

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Published in:Birth defects research. Part C. Embryo today 2010-06, Vol.90 (2), p.155-162
Main Authors: Knudsen, Thomas B., Kochhar, Devendra M.
Format: Article
Language:English
Subjects:
Animals
Chromosome Mapping
Ectromelia - genetics
Ectromelia - metabolism
Extremities - embryology
Female
Fetal Diseases - genetics
Fetal Diseases - metabolism
Humans
Introns
Limb Buds - embryology
Limb Buds - metabolism
limb development
Mesoderm - metabolism
Mice
mouse mutant
Mutation
Phenotype
Polydactyly - embryology
Polydactyly - genetics
Polydactyly - metabolism
Pregnancy
teratology
Toes
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Summary:Hemimelic extra toes (Hx) arose spontaneously as a dominant mutation in B10.D2/nSnJ mice in 1967. It specifically affects the appendicular skeleton, causing variable foreshortening of the tibia (radius) and preaxial polydactylism. Early anatomical studies revealed anterior overgrowth of the autopod, with decreased apoptosis and increased mitosis in the anterior apical ectodermal ridge and underlying mesenchyme; overextension of apoptosis in the central zeugopod accounted for hemimelia. The Hx mutant phenotype was coarsely mapped to mouse chromosome (Chr) 5 and closely linked to engrailed‐2 (En2) and Sonic hedgehog (Shh). This region is syntenic to human Chr 7q36 that harbors several dominant mutations affecting the hand. High‐resolution genome mapping identified the Hx mutation as a G → A base pair transition within Intron 5 of the murine Lmbr1 locus. The critical effect is on a multifunctional conserved regulatory element that acts as a limb‐specific, long‐distance cis‐acting enhancer of Shh expression. As such, the Hx mutant phenotype results from ectopic Shh signals at the anterior margin of the limb bud that directly or indirectly alter FGF4 signaling from the apical ectodermal ridge. Given significant advances in understanding of embryonic development in general and limb development in particular, this review article reveals how research that once attracted interest of teratologists has advanced across the decades to pinpoint a critical molecular lesion and reveal a potential mechanism of a specific malformation that is found commonly in experimental teratology. Birth Defects Research (Part C) 90:155–162, 2010. © 2010 Wiley‐Liss, Inc.
ISSN:1542-975X
1542-9768
DOI:10.1002/bdrc.20181