Predicting liver cyst severity by mutations in patients with autosomal-dominant polycystic kidney disease
- PMID: 33811288
- DOI: 10.1007/s12072-021-10176-9
Predicting liver cyst severity by mutations in patients with autosomal-dominant polycystic kidney disease
Abstract
Background: Most patients with autosomal-dominant polycystic kidney disease (ADPKD) develop liver cysts and polycystic liver disease as they age. To date, no simple clinical indicator has been confirmed to predict polycystic liver disease exacerbation. Furthermore, the effect of the type and location of mutation on disease progression of polycystic liver disease remains unclear. Here, we aimed to establish a simple liver cyst indicator for clinical practice and investigate whether gene mutations determined liver phenotype in patients with autosomal-dominant polycystic kidney disease.
Methods: In total, 129 patients with ADPKD were enrolled and liver cyst indicators were assessed based on mutation type (truncating mutation: nonsense, frameshift, and splicing mutation; non-truncating mutation: substitution) and mutation position. Liver cyst severity was determined using Gigot and Drenth classifications, based on their number, maximum diameter, and area ratio with the liver.
Results: We observed an overall prevalence of 62.8% for polycystic liver disease. Patients with PKD1 nonsense mutations, a type of PKD1 truncating mutation, exhibited more severe liver disease phenotypes than those without the mutation. We identified maximum diameter as a potential liver cyst indicator. Moreover, a subgroup analysis that included a PKD1 nonsense mutation cohort revealed that genetic mutations located closer to the 5' end of PKD1 were associated with a maximum diameter index value ≥ 6 cm.
Conclusion: PKD1 nonsense mutations were associated with liver cyst severity, which along with maximum diameter index as a simple clinical indicator for liver cysts, may improve the treatment of polycystic liver disease associated with ADPKD.
Keywords: Cyst-liver area ratio; Drenth classification; Gigot classification; Liver cyst indicator; Maximum liver cyst diameter; Mutation type; Nonsense mutation; PKD1; Polycystic liver disease; Polycystin-1; Sex difference; Substitution mutation.
© 2021. Asian Pacific Association for the Study of the Liver.
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