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Liver-restricted deletion of the biliary atresia candidate gene Pkd1l1 causes bile duct dysmorphogenesis and ciliopathy.

Dominick J HellenAshley BennettSudarshan R MallaCaroline KlindtAnuradha RaoPaul A DawsonSaul J Karpen
Published in: Hepatology (Baltimore, Md.) (2023)
Bile duct ligation of the Pkd1l1 -deficient mouse model mirrors several aspects of the intrahepatic pathophysiology of biliary atresia in humans including bile duct dysmorphogenesis, peribiliary fibroinflammation, hepatic arteriopathy, and ciliopathy. This first genetically linked model of biliary atresia, the Pkd1l1 LKO mouse, may allow researchers a means to develop a deeper understanding of the pathophysiology of this serious and perplexing disorder, including the opportunity to identify rational therapeutic targets.
Keyphrases
  • polycystic kidney disease
  • mouse model
  • copy number
  • genome wide
  • dna methylation
  • genome wide identification