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

The cerebellar morphological phenotype of the spontaneous neurological mutant mouse dreher ( Lmx1a dr - J ) results from cell fate changes in dorsal midline patterning involving the roof plate and rhombic lip. Positional cloning revealed that the gene Lmx1a , which encodes a LIM homeodomain protein,...

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Bibliographic Details
Published in:Brain Structure and Function 2014-01, Vol.219 (1), p.35-47
Main Authors: Sillitoe, Roy V., George-Jones, Nicholas A., Millen, Kathleen J., Hawkes, Richard
Format: Article
Language:English
Subjects:
Animals
Biomedical and Life Sciences
Biomedicine
Brain
Brain architecture
Cell Biology
Cellular biology
Cerebellum - abnormalities
Cerebellum - metabolism
Cerebellum - pathology
Developmental biology
Fructose-Bisphosphate Aldolase - metabolism
Gene Expression Regulation - genetics
Genes
Heat-Shock Proteins - metabolism
LIM-Homeodomain Proteins - genetics
Mice
Mice, Mutant Strains
Mutation
Mutation - genetics
Neoplasm Proteins - metabolism
Nerve Tissue Proteins - genetics
Nerve Tissue Proteins - metabolism
Neurology
Neurosciences
Original Article
Purkinje Cells - metabolism
Purkinje Cells - pathology
Rodents
Transcription Factors - genetics
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Summary:The cerebellar morphological phenotype of the spontaneous neurological mutant mouse dreher ( Lmx1a dr - J ) results from cell fate changes in dorsal midline patterning involving the roof plate and rhombic lip. Positional cloning revealed that the gene Lmx1a , which encodes a LIM homeodomain protein, is mutated in dreher , and is expressed in the developing roof plate and rhombic lip. Loss of Lmx1a causes reduction of the roof plate, an important embryonic signaling center, and abnormal cell fate specification within the embryonic cerebellar rhombic lip. In adult animals, these defects result in variable, medial fusion of the cerebellar vermis and posterior cerebellar vermis hypoplasia. It is unknown whether deleting Lmx1a results in displacement or loss of specific lobules in the vermis. To distinguish between an ectopic and absent vermis, the expression patterns of two Purkinje cell-specific compartmentation antigens, zebrin II/aldolase C and the small heat shock protein HSP25 were analyzed in dreher cerebella. The data reveal that despite the reduction in volume and abnormal foliation of the cerebellum, the transverse zones and parasagittal stripe arrays characteristic of the normal vermis are present in dreher , but may be highly distorted. In dreher mutants with a severe phenotype, zebrin II stripes are fragmented and distributed non-symmetrically about the cerebellar midline. We conclude that although Purkinje cell agenesis or selective Purkinje cell death may contribute to the dreher phenotype, our data suggest that aberrant anlage patterning and granule cell development lead to Purkinje cell ectopia, which ultimately causes abnormal cerebellar architecture in dreher .
ISSN:1863-2653
1863-2661
0340-2061
DOI:10.1007/s00429-012-0482-6