AI Article Synopsis

  • The study compares the quality of DNA derived from blood, saliva, and buccal samples for whole-genome sequencing (WGS).
  • Significant differences were found in sequencing quality metrics, with blood showing better results, especially for detecting copy number variants.
  • The findings suggest that blood-derived DNA is preferable for WGS, and if saliva or buccal samples are used, methylation-based enrichment should be avoided.

Article Abstract

Background: Whole blood is currently the most common DNA source for whole-genome sequencing (WGS), but for studies requiring non-invasive collection, self-collection, greater sample stability or additional tissue references, saliva or buccal samples may be preferred. However, the relative quality of sequencing data and accuracy of genetic variant detection from blood-derived, saliva-derived and buccal-derived DNA need to be thoroughly investigated.

Methods: Matched blood, saliva and buccal samples from four unrelated individuals were used to compare sequencing metrics and variant-detection accuracy among these DNA sources.

Results: We observed significant differences among DNA sources for sequencing quality metrics such as percentage of reads aligned and mean read depth (p<0.05). Differences were negligible in the accuracy of detecting short insertions and deletions; however, the false positive rate for single nucleotide variation detection was slightly higher in some saliva and buccal samples. The sensitivity of copy number variant (CNV) detection was up to 25% higher in blood samples, depending on CNV size and type, and appeared to be worse in saliva and buccal samples with high bacterial concentration. We also show that methylation-based enrichment for eukaryotic DNA in saliva and buccal samples increased alignment rates but also reduced read-depth uniformity, hampering CNV detection.

Conclusion: For WGS, we recommend using DNA extracted from blood rather than saliva or buccal swabs; if saliva or buccal samples are used, we recommend against using methylation-based eukaryotic DNA enrichment. All data used in this study are available for further open-science investigation.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6929712PMC
http://dx.doi.org/10.1136/jmedgenet-2019-106281DOI Listing

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