AI Article Synopsis

  • Human respiratory health is impacted by sex, with males facing a higher risk, and these differences are evident from birth, hinting at a genetic basis.
  • Research involved analyzing DNA methylation patterns in nasal samples from newborns and infants to identify sex-based genomic signatures linked to X-chromosome methylation.
  • The study found that X-linked genes exhibited varying methylation, with only about 50% showing significant differences between sexes, suggesting potential implications for future respiratory health and disease predisposition.

Article Abstract

Human respiratory conditions are largely influenced by the individual's sex resulting in overall higher risk for males. Sex-based respiratory differences are present at birth suggesting a strong genetic component. Our objective was to characterize early life sex-based genomic signatures determined by variable X-chromosome methylation in the airways. We compared male versus female genome-wide DNA methylation in nasal airway samples from newborns and infants aged 1-6 months (N = 12). We analyzed methylation signals across CpG sites mapped to each X-linked gene using an unsupervised classifier (principal components) followed by an internal evaluation and an exhaustive cross-validation. Results were validated in an independent population of children (N = 72) following the same algorithm. X-linked genes with significant sex-based differential methylation in the nasal airway of infants represented only about 50% of the unique protein coding transcripts. X-linked genes without significant sex-based differential methylation included genes with evidence of escaping X-inactivation and female-biased airway expression. These genes showed similar methylation patterns in males and females suggesting unbalanced X-chromosome dosage. In conclusion, we identified that the human airways have already sex-based DNA methylation signatures at birth. These early airway epigenomic marks may determine sex-based respiratory phenotypes and overall predisposition to develop respiratory disorders later in life.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5882800PMC
http://dx.doi.org/10.1038/s41598-018-23063-5DOI Listing

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