A genomic and bioinformatic-based approach to identify genetic variants for liver cancer across multiple continents.
Muhammad Ma'rufLalu Muhammad IrhamWirawan AdikusumaMade Ary SarasmitaSabiah KhairiBarkah Djaka PurwantoRockie ChongMaulida MazayaLalu Muhammad Harmain SiswantoPublished in: Genomics & informatics (2023)
Liver cancer is the fourth leading cause of death worldwide. Well-known risk factors include hepatitis B virus and hepatitis C virus, along with exposure to aflatoxins, excessive alcohol consumption, obesity, and type 2 diabetes. Genomic variants play a crucial role in mediating the associations between these risk factors and liver cancer. However, the specific variants involved in this process remain under-explored. This study utilized a bioinformatics approach to identify genetic variants associated with liver cancer from various continents. Single-nucleotide polymorphisms associated with liver cancer were retrieved from the genome-wide association studies catalog. Prioritization was then performed using functional annotation with HaploReg v4.1 and the Ensembl database. The prevalence and allele frequencies of each variant were evaluated using Pearson correlation coefficients. Two variants, rs2294915 and rs2896019, encoded by the PNPLA3 gene, were found to be highly expressed in the liver tissue, as well as in the skin, cell-cultured fibroblasts, and adipose-subcutaneous tissue, all of which contribute to the risk of liver cancer. We further found that these two SNPs (rs2294915 and rs2896019) were positively correlated with the prevalence rate. Positive associations with the prevalence rate were more frequent in East Asian and African populations. We highlight the utility of this population-specific PNPLA3 genetic variant for genetic association studies and for the early prognosis and treatment of liver cancer. This study highlights the potential of integrating genomic databases with bioinformatic analysis to identify genetic variations involved in the pathogenesis of liver cancer. The genetic variants investigated in this study are likely to predispose to liver cancer and could affect its progression and aggressiveness. We recommend future research prioritizing the validation of these variations in clinical settings.
Keyphrases
- copy number
- risk factors
- hepatitis b virus
- type diabetes
- genome wide
- hepatitis c virus
- insulin resistance
- alcohol consumption
- cardiovascular disease
- metabolic syndrome
- emergency department
- genome wide association
- body mass index
- dna methylation
- stem cells
- risk assessment
- human immunodeficiency virus
- glycemic control
- climate change
- weight loss
- physical activity
- mass spectrometry
- transcription factor
- rna seq
- wound healing