AI Article Synopsis

  • * A study on 48 infants examined how DNA methylation patterns in umbilical cord blood and placenta relate to weight measurements at six months, identifying 23 genes from cord blood and 10 from placenta linked to weight outcomes.
  • * Three specific genes (PLIN4, UBE2F, and PPP1R16B) showed strong associations with weight gain, and a new Methylation Risk Score was developed to identify infants at higher risk for obesity, paving the way for more targeted research in the future.

Article Abstract

Childhood obesity represents a significant global health concern and identifying its risk factors is crucial for developing intervention programs. Many "omics" factors associated with the risk of developing obesity have been identified, including genomic, microbiomic, and epigenomic factors. Here, using a sample of 48 infants, we investigated how the methylation profiles in cord blood and placenta at birth were associated with weight outcomes (specifically, conditional weight gain, body mass index, and weight-for-length ratio) at age six months. We characterized genome-wide DNA methylation profiles using the Illumina Infinium MethylationEpic chip, and incorporated information on child and maternal health, and various environmental factors into the analysis. We used regression analysis to identify genes with methylation profiles most predictive of infant weight outcomes, finding a total of 23 relevant genes in cord blood and 10 in placenta. Notably, in cord blood, the methylation profiles of three genes (PLIN4, UBE2F, and PPP1R16B) were associated with all three weight outcomes, which are also associated with weight outcomes in an independent cohort suggesting a strong relationship with weight trajectories in the first six months after birth. Additionally, we developed a Methylation Risk Score (MRS) that could be used to identify children most at risk for developing childhood obesity. While many of the genes identified by our analysis have been associated with weight-related traits (e.g., glucose metabolism, BMI, or hip-to-waist ratio) in previous genome-wide association and variant studies, our analysis implicated several others, whose involvement in the obesity phenotype should be evaluated in future functional investigations.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11268442PMC
http://dx.doi.org/10.1017/S2040174424000060DOI Listing

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