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Quantifying the benefit offered by transcript assembly with Scallop-LR on single-molecule long reads.


ABSTRACT: Single-molecule long-read sequencing has been used to improve mRNA isoform identification. However, not all single-molecule long reads represent full transcripts due to incomplete cDNA synthesis and sequencing length limits. This drives a need for long-read transcript assembly. By adding long-read-specific optimizations to Scallop, we developed Scallop-LR, a reference-based long-read transcript assembler. Analyzing 26 PacBio samples, we quantified the benefit of performing transcript assembly on long reads. We demonstrate Scallop-LR identifies more known transcripts and potentially novel isoforms for the human transcriptome than Iso-Seq Analysis and StringTie, indicating that long-read transcript assembly by Scallop-LR can reveal a more complete human transcriptome.

SUBMITTER: Tung LH 

PROVIDER: S-EPMC6918626 | biostudies-literature | 2019 Dec

REPOSITORIES: biostudies-literature

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Quantifying the benefit offered by transcript assembly with Scallop-LR on single-molecule long reads.

Tung Laura H LH   Shao Mingfu M   Kingsford Carl C  

Genome biology 20191218 1


Single-molecule long-read sequencing has been used to improve mRNA isoform identification. However, not all single-molecule long reads represent full transcripts due to incomplete cDNA synthesis and sequencing length limits. This drives a need for long-read transcript assembly. By adding long-read-specific optimizations to Scallop, we developed Scallop-LR, a reference-based long-read transcript assembler. Analyzing 26 PacBio samples, we quantified the benefit of performing transcript assembly on  ...[more]

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