Ectopic Hoxa-1 induces rhombomere transformation in mouse hindbrain

Ectopic Hoxa-1 induces rhombomere transformation in mouse hindbrain

Homeobox genes are expressed with a specific spatial and temporal order, which is essential for pattern formation during the early development of both invertebrates and vertebrates. Here we show that widespread ectopic expression of the Hoxa-1 (Hox 1.6) gene directed by a human beta-actin promoter i...

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Veröffentlicht in:Development (Cambridge) 1994-09, Vol.120 (9), p.2431-2442
Hauptverfasser: ZHANG, M, HEE-JOON KIM, MARSHALL, H, GENDRON-MAGUIRE, M, LUCAS, D. A, BARON, A, GUDAS, L. J, GRIDLEY, T, KRUMLAUF, R, GRIPPO, J. F
Format: Artikel
Sprache:eng
Schlagworte:
Actins - genetics
Animals
Base Sequence
Biological and medical sciences
Embryology: invertebrates and vertebrates. Teratology
Fundamental and applied biological sciences. Psychology
Gene Expression Regulation
Genes, Homeobox
Immunohistochemistry
In Situ Hybridization
Mice
Mice, Transgenic
Molecular embryology
Molecular Sequence Data
Morphogenesis - genetics
Nervous System - embryology
Neural Crest - cytology
Promoter Regions, Genetic
Rhombencephalon - embryology
Transformation, Genetic
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Zusammenfassung:Homeobox genes are expressed with a specific spatial and temporal order, which is essential for pattern formation during the early development of both invertebrates and vertebrates. Here we show that widespread ectopic expression of the Hoxa-1 (Hox 1.6) gene directed by a human beta-actin promoter in transgenic mice is embryolethal and produces abnormal phenotypes in a subset of domains primarily located in anterior regions. Interestingly, this abnormal development in the Hoxa-1 transgenic mice is associated with ectopic expression of the Hoxb-1 (Hox 2.9) gene in select hindbrain regions. At gestation day 9.5, two domains of strong Hoxb-1 expression are found in the anterior region of the hindbrains of Hoxa-1 transgenic embryos. One region represents the normal pattern of Hoxb-1 expression in rhombomere 4 and its associated migrating neural crest cells, while another major domain of Hoxb-1 expression consistently appears in rhombomere 2. Similar ectopic domains of beta-galactosidase activity are detected in dual transgenic embryos containing both beta-actin/Hoxa-1 transgene and a Hoxb-1/lacZ reporter construct. Expression of another lacZ reporter gene that directs beta-galactosidase activity predominantly in rhombomere 2 is suppressed in the Hoxa-1 transgenic embryos. We have also detected weaker and variable ectopic Hoxb-1 expression in rhombomeres 1, 3 and 6. No ectopic Hoxb-1 expression is detected in rhombomere 5 and the expression of Hoxa-3 and Krox-20 in this region is unchanged in the Hoxa-1 transgenic embryos. While no obvious change in the morphology of the trigeminal or facial-acoustic ganglia is evident, phenotypic changes do occur in neurons that emanate from rhombomeres 2 and 3 in the Hoxa-1 transgenic embryos. Additionally, alterations in the pattern of Hoxa-2 and Hoxb-1 expression in a subpopulation of neural crest cells migrating from the rhombomere 2 region are detected in these transgenics. Taken together, these data suggest that ectopic Hoxa-1 expression can reorganize select regions of the developing hindbrain by inducing partial transformations of several rhombomeres into a rhombomere-4-like identity.
ISSN:0950-1991
1477-9129
DOI:10.1242/dev.120.9.2431