BioTechniques (Oct 2014)

Next-generation sequencing of custom amplicons to improve coverage of HaloPlex multigene panels

  • Emily M. Coonrod,
  • Jacob D. Durtschi,
  • Chad VanSant Webb,
  • Karl V. Voelkerding,
  • Attila Kumánovics

DOI
https://doi.org/10.2144/000114217
Journal volume & issue
Vol. 57, no. 4
pp. 204 – 207

Abstract

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Next-generation sequencing (NGS) of multigene panels performed for genetic clinical diagnostics requires 100% coverage of all targeted genes. In the genetic diagnostics laboratory, coverage gaps are typically filled with Sanger sequencing after NGS data are collected and analyzed. Libraries prepared using the hybridization-based custom capture HaloPlex method are covered at ∼98% and include gaps in coverage because of the location of the restriction enzyme sites used for fragmentation and differences in the designed and actual library insert size. We describe a method for improving the coverage of HaloPlex libraries by generating a set of amplicons spanning known low-coverage regions that are pooled, indexed by sample, and sequenced together with the HaloPlex libraries. This approach reduces the number of post-NGS Sanger sequencing reactions required and complements any NGS library preparation method when complete gene coverage is necessary.

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