Literature DB >> 10842066

Dorsal patterning defects in the hindbrain, roof plate and skeleton in the dreher (dr(J)) mouse mutant.

M Manzanares1, P A Trainor, L Ariza-McNaughton, S Nonchev, R Krumlauf.   

Abstract

dreher is a spontaneous mouse mutation in which adult animals display a complex phenotype associated with hearing loss, neurological, pigmentation and skeletal abnormalities. During early embryogenesis, the neural tube of dreher mutants is abnormally shaped in the region of the rhomboencephalon, due to problems in the formation of a proper roof plate over the otic hindbrain. We have studied the expression of Hox/lacZ transgenic mouse strains in the dreher background and shown that primary segmentation of the neural tube is not altered in these mutants, although correct morphogenesis is affected resulting in misshapen rhombomeres. Neural crest derivatives from rhombomere 6, such as the glossopharyngeal ganglion, are defective, and the dorsal neural tube marker Wnt1 is absent from this segment. Selected trunk neural crest populations are also altered, as there is a lack of pigmentation in the thoracic region of mutant mice. Skeletal defects include abnormal cranial bones of neural crest origin, and improper fusion of the dorsal aspects of cervical and thoracic vertebrae. Taken together, the gene affected in the dreher mutant is responsible for correct patterning of the dorsal-most cell types of the neural tube, that is, the neural crest and the roof plate, in the hindbrain region. Axial skeletal defects could reflect inductive influence of the dorsal neural tube on proper fusion of the neural arches. It is possible that a common precursor population for both neural crest and roof plate is the cellular target of the dreher mutation.

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Year:  2000        PMID: 10842066     DOI: 10.1016/s0925-4773(00)00288-4

Source DB:  PubMed          Journal:  Mech Dev        ISSN: 0925-4773            Impact factor:   1.882


  10 in total

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2.  The transcription factor Zfp423/OAZ is required for cerebellar development and CNS midline patterning.

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4.  Interaction with ectopic cochlear crista sensory epithelium disrupts basal cochlear sensory epithelium development in Lmx1a mutant mice.

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5.  Purkinje cell compartmentalization in the cerebellum of the spontaneous mutant mouse dreher.

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8.  Lmx1a is required for segregation of sensory epithelia and normal ear histogenesis and morphogenesis.

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Journal:  Cell Tissue Res       Date:  2008-11-05       Impact factor: 5.249

9.  Zic1 and Zic4 regulate zebrafish roof plate specification and hindbrain ventricle morphogenesis.

Authors:  Gina E Elsen; Louis Y Choi; Kathleen J Millen; Yevgenya Grinblat; Victoria E Prince
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10.  Lmx1a maintains proper neurogenic, sensory, and non-sensory domains in the mammalian inner ear.

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  10 in total

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