Genes that cause severe liver disease in children also influence risk and severity of common liver conditions in adults
Abstract
Background and aims
Rare, pathogenic variants in multiple genes can cause severe liver disease, requiring transplantation in childhood, but it is unclear whether common variants in the same genes confer risk of liver disease in adults. Here, we aimed to establish whether ‘monogenic’ liver diseases are associated with a spectrum of liver phenotypes in adulthood.
Methods
We identified 99 genes where pathological mutations cause significant liver disease in children. For each, we used population-level data from over 1.5 million adults to identify associations with biomarkers of liver injury (e.g. ALT). These observations were validated using six external cohorts of adults with clinical liver disease and transcriptomics. Finally, we illustrated the importance of the JAG1-NOTCH pathway on the ductular reaction in adult liver disease using immunohistochemistry and transcriptomics.
Results
We identified 89 genome-wide (p<5x10-8) associations with biomarkers of liver injury in 46% (45/99) of genes. Variants inABCC2,ADK,ASL,BCS1L,HFE, andSERPINA1were also linked with presence of clinical liver disease in adults. For example, rs2862926C>T encoding p.Ile1324= inABCC2(which causes Dubin-Johnson syndrome) was associated with lower ALT (p=7.1x10-12) and lower risk of MASLD (p-FDR=0.03). Transcriptional expression of 30% of genes was associated with severity of MASLD. p.Pro871Arg in JAG1 causes a subtle form of Alagille syndrome with higher bilirubin (9.7x10-10) and hypertension (p=4.2x10-14). JAG1 and NOTCH2 were expressed in injured bile ducts but not adjacent unaffected ducts and transcriptional expression of JAG1 correlated with fibrosis stage in primary sclerosing cholangitis.
Conclusions
Pathways affected by severe childhood liver disease also influence risk and severity of liver disease in adulthood.
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