Chemical capping improves template switching and enhances sequencing of small RNAs

Nucleic Acids Res. 2022 Jan 11;50(1):e2. doi: 10.1093/nar/gkab861.

Abstract

Template-switching reverse transcription is widely used in RNA sequencing for low-input and low-quality samples, including RNA from single cells or formalin-fixed paraffin-embedded (FFPE) tissues. Previously, we identified the native eukaryotic mRNA 5' cap as a key structural element for enhancing template switching efficiency. Here, we introduce CapTS-seq, a new strategy for sequencing small RNAs that combines chemical capping and template switching. We probed a variety of non-native synthetic cap structures and found that an unmethylated guanosine triphosphate cap led to the lowest bias and highest efficiency for template switching. Through cross-examination of different nucleotides at the cap position, our data provided unequivocal evidence that the 5' cap acts as a template for the first nucleotide in reverse transcriptase-mediated post-templated addition to the emerging cDNA-a key feature to propel template switching. We deployed CapTS-seq for sequencing synthetic miRNAs, human total brain and liver FFPE RNA, and demonstrated that it consistently improves library quality for miRNAs in comparison with a gold standard template switching-based small RNA-seq kit.

Publication types

  • Research Support, Non-U.S. Gov't

MeSH terms

  • Humans
  • RNA / analysis*
  • RNA Caps / metabolism*
  • Sequence Analysis, RNA / methods*
  • Tissue Fixation

Substances

  • RNA Caps
  • RNA