Abstract
BackgroundSingle nucleotide polymorphisms (SNPs) in genes including PNPLA3, TM6SF2, HSD17B13 and SERPINA1 have been identified as risk modifiers of progression in chronic liver disease (CLD). However, it is unclear whether genotyping for these risk variants is useful in clinical routine. MethodsLiver disease severity was assessed by liver stiffness measurement (LSM) and by presence of clinical manifestations of advanced-chronic liver disease (ACLD) in 779 consecutive CLD patients at the time of referral to a tertiary center. The associations of risk variants with CLD severity were calculated individually and in a combined model using a polygenic risk-score. ResultsNon-alcoholic fatty liver disease (NAFLD) was the most common etiology (n = 511, 65.6%), and ACLD was present in 217 (27.9%) patients. The PNPLA3-G-allele remained independently associated with higher LSM (adjusted-B: 2.508 [95%CI: 0.887–4.130], P = 0.002) or the presence of ACLD (aOR: 1.562 [95%CI: 1.097–2.226], P = 0.013). SERPINA1-Z-allele was also independently associated with LSM (adjusted-B: 4.558 [95%CI: 1.182–7.934], P = 0.008), while the other risk alleles did not attain statistical significance. Combining these risk alleles into a polygenic risk-score was significantly associated with LSM (adjusted-B: 0.948 [95%CI: 0.153–1.743], P = 0.020). ConclusionPNPLA3 risk-variants are linked to liver disease severity at the time of first referral to an outpatient hepatology clinic.
Highlights
Several single nucleotide polymorphisms (SNPs) have been identified and confirmed to modify the risk of progression in chronic liver disease (CLD) of different etiologies
We identified a different distribution of PNPLA3 variants in our cohort when compared to an ideal population in HardyWeinberg-equilibrium while their distribution was not different for HSD17B13, TM6SF2, and SERPINA1
The prevalence of PNPLA3 risk allele in our cohort was higher than reported in literature while it was similar for TM6SF2, HSD17B13 and SERPINA1 [ 14, 26 ]
Summary
Several single nucleotide polymorphisms (SNPs) have been identified and confirmed to modify the risk of progression in chronic liver disease (CLD) of different etiologies. It has been shown to increase the progression to cirrhosis in prevalent (PNPLA3, SERPINA1) and less prevalent (HSD17B13) in advanced stages [14–18]. We aimed at investigating the usefulness of genotyping for four important SNPs (PNPLA3, TM6SF2, HSD17B13, SERPINA1) in clinical routine for the assessment of the severity of CLD. Single nucleotide polymorphisms (SNPs) in genes including PNPLA3, TM6SF2, HSD17B13 and SERPINA1 have been identified as risk modifiers of progression in chronic liver disease (CLD). It is unclear whether genotyping for these risk variants is useful in clinical routine
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