[No authors listed]
Glutamine dependence is a unique metabolic defect seen in cutaneous melanoma (CM), directly influencing the treatment and prognosis. Here, we investigated the associations between 6025 common single-nucleotide polymorphisms (SNPs) in 77 glutamine metabolic pathway genes with CM-specific survival (CMSS) using genotyping datasets from two published genome-wide association studies (GWASs). In the single-locus analysis, 76 SNPs were found to be significantly associated with CMSS (Pâ<â.050, false-positive report probabilityâ<â0.2 and Bayesian false discovery probabilityâ<â0.8) in the discovery dataset, of which seven SNPs were replicated in the validation dataset and three SNPs (HAL rs17676826Tâ>âC, LGSN rs12663017Tâ>âA, and NOXRED1 rs8012548Aâ>âG) independently predicted CMSS, with an effect-allele attributed adjusted hazards ratio of 1.52 (95% confidence intervalâ=â1.19-1.93) and Pâ<â.001, 0.68 (0.54-0.87) and Pâ=â.002 and 0.62 (0.46-0.83) and Pâ=â.002, respectively. The model including the number of unfavorable genotypes (NUGs) of these three SNPs and covariates improved the five-year CMSS prediction (Pâ=â.012) than the one with other covariates only. Further expression quantitative trait loci (eQTL) analysis found that the LGSN rs12663017 A allele was significantly associated with increased messenger RNA (mRNA) expression levels (Pâ=â8.89âÃâ10 -11 ) in lymphoblastoid cell lines of the database. In the analysis of the genotype tissue expression (GTEx) project datasets, HAL rs17676826 C and NOXRED1 rs8012548 G alleles were significantly associated with their mRNA expression levels in sun-exposed skin of the lower leg (Pâ=â6.62âÃâ10-6 and 1.37âÃâ10-7 , respectively) and in sun-not-exposed suprapubic skin (Pâ<â.001 and 1.43âÃâ10-8 , respectively). Taken together, these genetic variants of glutamine-metabolic pathway genes may be promising predictors of survival in patients with CM.
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