Official Title
Coordinating Center- Mapping Disease Pathways for Biliary Atresia
Brief Title
Mapping Disease Pathways for Biliary Atresia
Protocol ID
NCT03273049
Lead Sponsor
University of Pittsburgh
Brief Summary
This project will primarily evaluate the developmental/genetic basis of biliary atresia,
the most common cause of liver failure at birth, and which accounts of half of all liver
transplants performed worldwide in children.
Detailed Description
Characterized by failure to drain bile from the liver due to atretic extrahepatic bile
ducts, BA is corrected in less than half of all affected children with surgical
reconstruction. The remainder progress to cirrhosis and require liver transplantation.
Because bile duct loss can be accompanied by other birth defects such as laterality
defects of the gut and cardiovascular systems, the disease has been categorized into the
more common 'isolated' variety presumably due to a perinatal viral cholangitis, and the
'syndromic' variety, due to genetic factors. Mechanistic differences implied by this
categorization have not been demonstrated conclusively. In contrast, three susceptibility
genes identified in predominantly 'isolated" BA cases, and the presence of abnormal cilia
which are known to predispose to laterality defects, in both isolated and syndromic forms
of BA suggest that in addition to environmental influences, genetic susceptibility is
important in both forms of BA. This view is reinforced by our preliminary work which
shows that knockdown of a novel BA susceptibility gene causes both biliary dysgenesis and
laterality defects in animal models. This finding also suggests that common birth defects
affecting the liver and other organs may originate from defects in the same genes. The
project will combine candidate gene identification and replication with human DNA samples
from 1100 BA subjects and their biological parents or siblings, if available, with
validation using corresponding human BA liver tissue and zebrafish knockdown models.
The project outcome will consist of pathways comprising multiple susceptibility genes
involved in morphogenesis of the liver and other organs, which explain the complex
phenotype of BA. The project will use the experimental and bioinformatics capabilities of
the Universities of Pittsburgh and California (at San Diego) to analyze data and study
human samples from the participating centers. Four of the world's largest pediatric liver
transplant centers, the Children's Hospitals of Pittsburgh (CHP), King's College Hospital
(KCH), London, UK, Birmingham Children's Hospital, UK (BCH), and the Hospital Sirio
Libanes (HSL), Sao Paulo, Brazil will enroll biliary atresia subjects and their
biological parents and/or siblings, if available.
Information developed in this project will be the basis for designing novel management
strategies to reduce the societal impact of this rare childhood disease.
Study Period
-
Enrollment Count
1,100 participants
Eligibility Criteria
Inclusion Criteria:
- living individuals who were diagnosed with Biliary Atresia and received or are about
to receive a liver transplant from multiple participating centers (Children's
Hospital of Pittsburgh, Kings College Hospital, Children's Hospital of Birmingham,
and Hospital Sírio-Libanês).
Exclusion Criteria:
- No child participant in the care of the state will be enrolled, nor will patients in
the care of temporary or informal guardians be enrolled
Filters
Biliary Atresia
RECRUITING
CHILD
ADULT
OLDER_ADULT