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A Combination of Single Nucleotide Polymorphisms is Associated with the Interindividual Variability of Cholesterol Bioavailability in Healthy Adult Males. | LitMetric

AI Article Synopsis

  • - The study investigates how genetic factors contribute to differences in cholesterol bioavailability among individuals, focusing on the combination of specific genetic variations (SNPs) rather than analyzing them one by one.
  • - Researchers conducted an experiment on 39 healthy men by measuring their plasma cholesterol levels after consuming a cholesterol-rich snack, revealing significant variability in their responses.
  • - A model including eight specific SNPs was found to explain nearly 60% of the differences in cholesterol absorption, indicating that certain genetic profiles may influence how well individuals utilize dietary cholesterol.

Article Abstract

Scope: Cholesterol bioavailability displays a high interindividual variability, partly due to genetic factors. Existing studies have focused on single nucleotide polymorphisms (SNPs) analyzed individually, which only explained a minor fraction of the variability of this complex phenotype. The aim is to identify a combination of SNPs associated with a significant part of the variability in cholesterol bioavailability.

Methods And Results: Thirty-nine healthy adult males are given a standard test snack containing 80 mg heptadeuterated (D7) cholesterol. The plasma D7-cholesterol concentration is measured at equilibrium 40 h after test snack intake. The D7-cholesterol response (D7-cholesterol/total cholesterol concentration) exhibits a relatively high interindividual variability (CV = 32%). The association of exonic SNPs in candidate genes (188 genes involved in or related to cholesterol metabolism) with the plasma D7-cholesterol response is assessed by univariate statistics followed by partial least squares regression. A significant model (p-value after cross-validation ANOVA = 1.64 × 10 ) that includes 8 SNPs (SOAT2-rs9658625, DNAH11-rs11768670, LIPC-rs690, MVK-rs2287218, GPAM-rs10787428, APOE-rs7412, CBS-rs234706, and WRN-rs1801196) explains 59.7% of the variance in cholesterol bioavailability (adjusted R²).

Conclusion: Here a combination of SNPs is significantly associated with the variability in dietary cholesterol bioavailability in healthy adult males.

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Source
http://dx.doi.org/10.1002/mnfr.202000480DOI Listing

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