| Literature DB >> 33804385 |
Georg Semmler1,2,3, Lorenz Balcar1,2, Hannes Oberkofler4, Stephan Zandanell1, Michael Strasser1, David Niederseer5, Alexandra Feldman1, Felix Stickel6, Pavel Strnad7, Christian Datz3, Bernhard Paulweber1, Elmar Aigner1.
Abstract
Single nucleotide polymorphisms (SNPs), including PNPLA3 rs738409 and SERPINA1 rs17580, have been identified as risk modifiers in the progression fatty liver disease (alcoholic (ALD) or non-alcoholic (NAFLD)). While PNPLA3 has been studied in various settings, the value of both SNPs has so far not been addressed in a real-world cohort of subjects referred for a diagnostic work-up of liver disease. Thus, liver disease severity was assessed in 1257 consecutive patients with suspected ALD or NAFLD at the time of referral to a tertiary center. Advanced chronic liver disease (ACLD) was present in 309 (24.6%) patients and clinically significant portal hypertension (CSPH) was present in 185 (14.7%) patients. The PNPLA3 G-allele was independently associated with a higher liver stiffness measurement (LSM; adjusted B: 2.707 (1.435-3.979), p < 0.001), and higher odds of ACLD (adjusted odds ratio (aOR): 1.971 (1.448-2.681), p < 0.001) and CSPH (aOR: 1.685 (1.180-2.406), p = 0.004). While the SERPINA1 Z-allele was not associated with a higher LSM or the presence of ACLD, it was independently associated with higher odds of CSPH (aOR: 2.122 (1.067-4.218), p = 0.032). Associations of the PNPLA3 G-allele and the SERPINA1 Z-allele with CSPH were maintained independently of each other. The presence of both risk variants further increased the likelihood of ACLD and CSPH.Entities:
Keywords: ALD; NAFLD; PNPLA3; SERPINA1; advanced chronic liver disease; cirrhosis
Year: 2021 PMID: 33804385 PMCID: PMC7999282 DOI: 10.3390/jpm11030165
Source DB: PubMed Journal: J Pers Med ISSN: 2075-4426