BMC Research Notes (Jul 2023)

A capture methyl-seq protocol with improved efficiency and cost-effectiveness using pre-pooling and enzymatic conversion

  • Keita Hasegawa,
  • Kazuhiko Nakabayashi,
  • Keisuke Ishiwata,
  • Yoshifumi Kasuga,
  • Kenichiro Hata,
  • Mamoru Tanaka

DOI
https://doi.org/10.1186/s13104-023-06401-3
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 6

Abstract

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Abstract Objective The opportunities for sequencing-based methylome analysis of clinical samples are increasing. To reduce its cost and the amount of genomic DNA required for library preparation, we aimed to establish a capture methyl-seq protocol, which adopts pre-pooling of multiple libraries before hybridization capture and TET2/APOBEC-mediated conversion of unmethylated cytosine to thymine. Results We compared a publicly available dataset generated by the standard Agilent protocol of SureSelect XT Human Methyl-Seq Kit and our dataset obtained by our modified protocol, EMCap, that adopted sample pre-pooling and enzymatic conversion. We confirmed that the quality of DNA methylation data was comparable between the two datasets. As our protocol, EMCap, is more cost-effective and reduces the amount of input genomic DNA, it would serve as a better choice for clinical methylome sequencing.

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