PUBLICATION

Cdx-Hox code controls competence for responding to Fgfs and retinoic acid in zebrafish neural tissue

Authors
Shimizu, T., Bae, Y.K., and Hibi, M.
ID
ZDB-PUB-061108-8
Date
2006
Source
Development (Cambridge, England)   133(23): 4709-4719 (Journal)
Registered Authors
Bae, Young Ki, Hibi, Masahiko, Shimizu, Takashi
Keywords
caudal-related genes, hox, Hindbrain, Fibroblast growth factor, Retinoic acid, Zebrafish
MeSH Terms
  • Rhombencephalon/drug effects
  • Rhombencephalon/embryology*
  • Rhombencephalon/metabolism
  • Gene Targeting
  • Transcription Factors/deficiency
  • Transcription Factors/genetics
  • Transcription Factors/metabolism
  • Genes, Homeobox
  • Tretinoin/pharmacology
  • Animals
  • Signal Transduction
  • Zebrafish/embryology*
  • Zebrafish/genetics
  • Zebrafish/metabolism
  • Spinal Cord/drug effects
  • Spinal Cord/embryology
  • Spinal Cord/metabolism
  • Zebrafish Proteins/deficiency
  • Zebrafish Proteins/genetics
  • Zebrafish Proteins/metabolism
  • Gene Expression Regulation, Developmental
  • Homeodomain Proteins/genetics
  • Homeodomain Proteins/metabolism
  • Fibroblast Growth Factors/pharmacology
(all 24)
PubMed
17079270 Full text @ Development
Abstract
Fibroblast growth factor (Fgf) and retinoic acid (RA) signals control the formation and anteroposterior patterning of posterior hindbrain. They are also involved in development processes in other regions of the embryo. Therefore, responsiveness to Fgf and RA signals must be controlled in a context-dependent manner. Inhibiting the caudal-related genes cdx1a and cdx4 in zebrafish embryos caused ectopic expression of genes that are normally expressed in the posterior hindbrain and anterior spinal cord, and ectopic formation of the hindbrain motor and commissure neurons in the posteriormost neural tissue. Combinational marker analyses suggest mirror-image duplication in the Cdx1a/4-defective embryos, and cell transplantation analysis further revealed that Cdx1a and Cdx4 repress a posterior hindbrain-specific gene expression cell-autonomously in the posterior neural tissue. Expression of fgfs and retinaldehyde dehydrogenase 2 suggested that in the Cdx1a/4-defective embryos, the Fgf and RA signaling activities overlap in the posterior body and display opposing gradients, compared with those in the hindbrain region. We found that Fgf and RA signals were required for ectopic expression. Expression of the posterior hox genes hoxb7a, hoxa9a or hoxb9a, which function downstream of Cdx1a/4, or activator fusion genes of hoxa9a or hoxb9a (VP16-hoxa9a, VP16-hoxb9a) suppressed this loss-of-function phenotype. These data suggest that Cdx suppresses the posterior hindbrain fate through regulation of the posterior hox genes; the posterior Hox proteins function as transcriptional activators and indirectly repress the ectopic expression of the posterior hindbrain genes in the posterior neural tissue. Our results indicate that the Cdx-Hox code modifies tissue competence to respond to Fgfs and RA in neural tissue.
Genes / Markers
Figures
Figure Gallery (12 images) / 2
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Expression
Gene Antibody Fish Conditions Stage Qualifier Anatomy Assay Figure
alcamazn-5WTstandard conditionsProtruding-mouthIHC
alcamazn-5WTstandard conditionsProtruding-mouthIHC
alcamazn-5WT + MO1-cdx1a + MO1-cdx4standard conditionsProtruding-mouthIHC
alcamazn-5WT + MO1-cdx1a + MO1-cdx4standard conditionsProtruding-mouthIHC
aldh1a2WTstandard conditions5-9 somitesISH
aldh1a2WTstandard conditions5-9 somitesISH
aldh1a2WTstandard conditions75%-epibolyISH
aldh1a2WT + MO1-cdx1astandard conditions5-9 somitesISH
aldh1a2WT + MO1-cdx1astandard conditions5-9 somitesISH
aldh1a2WT + MO1-cdx1astandard conditions75%-epibolyISH
1 - 10 of 167
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Phenotype
Fish Conditions Stage Phenotype Figure
WT + MO1-cdx1a + MO1-cdx4standard conditions26+ somites
WT + MO1-cdx1a + MO1-cdx4standard conditions26+ somites
WT + MO1-cdx1a + MO1-cdx4standard conditionsLong-pec
WT + MO1-cdx1a + MO1-cdx4standard conditionsProtruding-mouth
WT + MO1-cdx1a + MO1-cdx4standard conditionsProtruding-mouth
WT + MO1-cdx1a + MO1-cdx4standard conditionsProtruding-mouth
1 - 6 of 6
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Mutations / Transgenics
Allele Construct Type Affected Genomic Region
rw0TgTransgenic Insertion
    1 - 1 of 1
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    Human Disease / Model
    No data available
    Sequence Targeting Reagents
    Target Reagent Reagent Type
    aldh1a2MO2-aldh1a2MRPHLNO
    cdx1aMO1-cdx1aMRPHLNO
    cdx4MO1-cdx4MRPHLNO
    fgf3MO5-fgf3MRPHLNO
    fgf8aMO3-fgf8aMRPHLNO
    wnt3aMO1-wnt3aMRPHLNO
    wnt8aMO1-wnt8aMRPHLNO
    wnt8aMO2-wnt8aMRPHLNO
    1 - 8 of 8
    Show
    Fish
    Fish
    rw0Tg
    WT
    WT + MO1-cdx1a
    WT + MO1-cdx1a + MO1-cdx4
    WT + MO1-cdx1a + MO1-cdx4 + MO1-wnt3a + MO1-wnt8a + MO2-wnt8a
    WT + MO1-cdx1a + MO1-cdx4 + MO2-aldh1a2
    WT + MO1-cdx1a + MO1-cdx4 + MO3-fgf8a + MO5-fgf3
    WT + MO1-cdx4
    WT + MO2-aldh1a2
    WT + MO3-fgf8a + MO5-fgf3
    1 - 10 of 10
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    Antibodies
    Orthology
    No data available
    Engineered Foreign Genes
    Marker Marker Type Name
    GFPEFGGFP
    1 - 1 of 1
    Show
    Mapping
    No data available
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    Citation
    Shimizu, T., Bae, Y.K., and Hibi, M. (2006) Cdx-Hox code controls competence for responding to Fgfs and retinoic acid in zebrafish neural tissue. Development (Cambridge, England). 133(23):4709-4719.