AI Article Synopsis
- Disorders of lipoprotein metabolism are key risk factors for cardiovascular disease, and genetic variations (SNPs) influence blood lipid profiles and responses to treatments.
- A study analyzed 34 SNPs in two groups: individuals not on lipid-lowering treatment (125 participants) and those taking statins (302 participants) to assess their lipid traits.
- Findings revealed specific SNPs linked to lipid traits in both groups, with an interesting connection to a favorable blood lipid profile associated with one particular SNP (rs3746444), indicating genetic variability in lipid management and treatment response.
Article Abstract
Disorders of lipoprotein metabolism are among the major risk factors for cardiovascular disease (CVD) development. Single nucleotide polymorphisms (SNPs) have been associated with the individual variability in blood lipid profile and response to lipid-lowering treatments. Here, we genotyped 34 selected SNPs located in coding genes related to lipid metabolism, inflammation, coagulation, and a polymorphism in the gene-a microRNA previously linked to CVD-to evaluate the association with lipid trait in subjects with moderate dyslipidemia not on lipid-lowering treatment (Treatment-naïve (TN) cohort, = 125) and in patients treated with statins (STAT cohort, = 302). We also explored the association between SNPs and the effect of a novel phytochemical lipid-lowering treatment in the TN cohort. We found that 6 SNPs (in the , TNFA, CETP, SOD2, and VEGFA genes) were associated with lipid traits in the TN cohort, while no association was found with the response to twelve-week phytochemical treatment. In the STAT cohort, nine SNPs (in the , CETP, CYP2C9, IL6, ABCC2, PON1, IL10, and VEGFA genes) were associated with lipid traits, three of which were in common with the TN cohort. Interestingly, in both cohorts, the presence of the rs3746444 SNP was associated with a more favorable blood lipid profile. Our findings could add information to better understand the individual genetic variability in maintaining a low atherogenic lipid profile and the response to different lipid-lowering therapies.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9145435 | PMC |
| http://dx.doi.org/10.3390/ijms23105617 | DOI Listing |
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