Publication | Open Access
Pseudouridines have context-dependent mutation and stop rates in high-throughput sequencing
45
Citations
30
References
2018
Year
GeneticsRna SplicingMolecular BiologyTranscriptomics TechnologyPseudouridine SitesGenomicsHigh Throughput SequencingTranscriptional RegulationReverse Transcription ConditionsLong Non-coding RnaGenome EngineeringTranscriptomicsMolecular DiagnosticsRna ProcessingDna SequencingReverse Transcription StopsRna Structure PredictionRna BiologyDna ReplicationRna SequencingGene ExpressionBioinformaticsFunctional GenomicsSequencingLong-read SequencingNatural SciencesNext-generation SequencingContext-dependent MutationMedicineGenome EditingSequence Assembly
The abundant RNA modification pseudouridine (Ψ) has been mapped transcriptome-wide by chemically modifying pseudouridines with carbodiimide and detecting the resulting reverse transcription stops in high-throughput sequencing. However, these methods have limited sensitivity and specificity, in part due to the use of reverse transcription stops. We sought to use mutations rather than just stops in sequencing data to identify pseudouridine sites. Here, we identify reverse transcription conditions that allow read-through of carbodiimide-modified pseudouridine (CMC-Ψ), and we show that pseudouridines in carbodiimide-treated human ribosomal RNA have context-dependent mutation and stop rates in high-throughput sequencing libraries prepared under these conditions. Furthermore, accounting for the context-dependence of mutation and stop rates can enhance the detection of pseudouridine sites. Similar approaches could contribute to the sequencing-based detection of many RNA modifications.
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