Abstract
Background Nonsense-mediated mRNA decay (NMD) is a eukaryotic, translation-dependent degradation pathway that targets mRNAs with premature termination codons and also regulates the expression of some mRNAs that encode full-length proteins. Although many genes express NMD-sensitive transcripts, identifying them based on short-read sequencing data remains a challenge.
Results To identify and analyze endogenous targets of NMD, we applied cDNA Nanopore sequencing and short-read sequencing to human cells with varying expression levels of NMD factors. Our approach detects full-length NMD substrates that are highly unstable and increase in levels or even only appear when NMD is inhibited. Among the many new NMD-targeted isoforms that our analysis identified, most derive from alternative exon usage. The isoform-aware analysis revealed many genes with significant changes in splicing but no significant changes in overall expression levels upon NMD knockdown. NMD-sensitive mRNAs have more exons in the 3΄UTR and, for those mRNAs with a termination codon in the last exon, the length of the 3΄UTR per se does not correlate with NMD sensitivity. Analysis of splicing signals reveals isoforms where NMD has been co-opted in the regulation of gene expression, though the main function of NMD seems to be ridding the transcriptome of isoforms resulting from spurious splicing events.
Conclusions Long-read sequencing enabled the identification of many novel NMD-sensitive mRNAs and revealed both known and unexpected features concerning their biogenesis and their biological role. Our data provide a highly valuable resource of human NMD transcript targets for future genomic and transcriptomic applications.
Competing Interest Statement
The authors have declared no competing interest.
Footnotes
Figures 2 and 4 were updated to include additional analysis and small modifications/clarifications to the text have been added. A list of pairs of NMD-sensitive and insensitive isoforms is included as a supplementary table.
Abbreviations
- NMD
- Nonsense-mediated mRNA decay
- AS-NMD
- Alternative splicing linked to NMD
- EJC
- Exon junction complex
- KD
- Knockdown
- dKD
- Double knockdown
- TC
- Termination codon
- PTC
- Premature termination codon
- PSI
- Percent spliced in
- ORF
- Open reading frame
- uORF
- Upstream open reading frame