PUBLICATION

A genetic screen in zebrafish identifies the mutants vps18, nf2 and foie gras as models of liver disease

Authors
Sadler, K.C., Amsterdam, A., Soroka, C., Boyer, J., and Hopkins, N.
ID
ZDB-PUB-050711-9
Date
2005
Source
Development (Cambridge, England)   132(15): 3561-3572 (Journal)
Registered Authors
Amsterdam, Adam, Hopkins, Nancy, Sadler Edepli, Kirsten C.
Keywords
Hepatomegaly, Biliary paucity, Choledochal cyst, Steatosis, Hepatogenesis, Zebrafish
MeSH Terms
  • Neurofibromin 2/genetics*
  • Base Sequence
  • Hepatomegaly/genetics*
  • Hepatocytes/cytology
  • Hepatocytes/physiology
  • Liver Diseases/embryology
  • Liver Diseases/genetics*
  • Zebrafish Proteins/genetics*
  • Fatty Liver/genetics*
  • Disease Models, Animal
  • Genetic Testing
  • Mutation*
  • Animals
  • Reverse Transcriptase Polymerase Chain Reaction
  • Zebrafish/embryology
  • Zebrafish/genetics*
  • DNA Primers
  • Ubiquitin-Protein Ligases/genetics*
  • Morphogenesis
(all 19)
PubMed
16000385 Full text @ Development
Abstract
Hepatomegaly is a sign of many liver disorders. To identify zebrafish mutants to serve as models for hepatic pathologies, we screened for hepatomegaly at day 5 of embryogenesis in 297 zebrafish lines bearing mutations in genes that are essential for embryonic development. Seven mutants were identified, and three have phenotypes resembling different liver diseases. Mutation of the class C vacuolar protein sorting gene vps18 results in hepatomegaly associated with large, vesicle-filled hepatocytes, which we attribute to the failure of endosomal-lysosomal trafficking. Additionally, these mutants develop defects in the bile canaliculi and have marked biliary paucity, suggesting that vps18 also functions to traffic vesicles to the hepatocyte apical membrane and may play a role in the development of the intrahepatic biliary tree. Similar findings have been reported for individuals with arthrogryposis-renal dysfunction-cholestasis (ARC) syndrome, which is due to mutation of another class C vps gene. A second mutant, resulting from disruption of the tumor suppressor gene nf2, develops extrahepatic choledochal cysts in the common bile duct, suggesting that this gene regulates division of biliary cells during development and that nf2 may play a role in the hyperplastic tendencies observed in biliary cells in individuals with choledochal cysts. The third mutant is in the novel gene foie gras, which develops large, lipid-filled hepatocytes, resembling those in individuals with fatty liver disease. These mutants illustrate the utility of zebrafish as a model for studying liver development and disease, and provide valuable tools for investigating the molecular pathogenesis of congenital biliary disorders and fatty liver disease.
Genes / Markers
Figures
Figure Gallery (8 images)
Show all Figures
Expression
Gene Antibody Fish Conditions Stage Qualifier Anatomy Assay Figure
trappc11trappc11hi1532bTgstandard conditionsDay 5Not DetectedRTPCR
trappc11WTstandard conditionsDay 5RTPCR
vps18vps18hi2499aTgstandard conditions1-cell to Day 5RTPCR
vps18vps18hi2499aTgstandard conditionsDay 5RTPCR
vps18WTstandard conditions1-cell to Day 5RTPCR
vps18WTstandard conditionsDay 5RTPCR
1 - 6 of 6
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Phenotype
Fish Conditions Stage Phenotype Figure
WT + MO1-vps18standard conditionsLong-pec
WT + MO1-vps18standard conditionsLong-pec
WT + MO1-vps18standard conditionsDay 5
cwc25hi1858aTgstandard conditionsDay 5
nf2bhi3332Tgstandard conditionsDay 5
nf2bhi3332Tgstandard conditionsDay 5
nf2bhi3332Tgstandard conditionsDays 7-13
nf2bhi3332Tgstandard conditionsDays 7-13
nf2bhi3332Tgstandard conditionsDays 7-13
nf2bhi3332Tgstandard conditionsDays 7-13
1 - 10 of 35
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Mutations / Transgenics
Allele Construct Type Affected Genomic Region
hi1134TgTransgenic Insertion
hi1532bTgTransgenic Insertion
hi1858aTgTransgenic Insertion
hi2499aTgTransgenic Insertion
hi3237TgTransgenic Insertion
hi3332TgTransgenic Insertion
hi3785TgTransgenic Insertion
1 - 7 of 7
Show
Human Disease / Model
Human Disease Fish Conditions Evidence
choledochal cystnf2bhi3332Tgstandard conditionsTAS
cholestasisvps18hi2499aTgstandard conditionsTAS
steatotic liver diseasetrappc11hi1532bTgstandard conditionsTAS
1 - 3 of 3
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Sequence Targeting Reagents
Target Reagent Reagent Type
nf2bMO1-nf2bMRPHLNO
trappc11MO1-trappc11MRPHLNO
vps18MO1-vps18MRPHLNO
1 - 3 of 3
Show
Fish
Fish
cwc25hi1858aTg
nf2bhi3332Tg
sox9ahi1134Tg
thoc2hi3237Tg
trappc11hi1532bTg
tubg1hi3785Tg
vps18hi2499aTg
WT
WT + MO1-vps18
1 - 9 of 9
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Antibodies
No data available
Orthology
Gene Orthology
vps18
1 - 1 of 1
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Engineered Foreign Genes
No data available
Mapping
No data available
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Citation
Sadler, K.C., Amsterdam, A., Soroka, C., Boyer, J., and Hopkins, N. (2005) A genetic screen in zebrafish identifies the mutants vps18, nf2 and foie gras as models of liver disease. Development (Cambridge, England). 132(15):3561-3572.