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SRX13128768: MCPyV tumor - viral reads; polyA illumina sequencing
1 ILLUMINA (Illumina NovaSeq 6000) run: 3,119 spots, 928,256 bases, 389,391b downloads

Design: MCPyV tumor - viral reads; polyA illumina sequencing
Submitted by: Dana-Farber Cancer Institute
Study: The Transcriptome Architecture of Polyomaviruses
show Abstracthide Abstract
Polyomaviruses (PyV) are ubiquitous pathogens that can cause devastating human diseases. Due to the small size of their genomes, PyV utilize complex patterns of RNA splicing to maximize their coding capacity. Despite the importance of PyV to human disease, their transcriptome architecture is poorly characterized. Here, we compare short- and long-read RNA sequencing data from eight human and non-human PyV. We provide a detailed transcriptome atlas for BK polyomavirus (BKPyV), an important human pathogen, and the prototype PyV, simian virus 40 (SV40). We identify pervasive wraparound transcription in PyV, wherein transcription runs through the polyA site and circles the genome multiple times. Comparative analyses identify novel, conserved transcripts that increase PyV coding capacity. One of these conserved transcripts encodes superT, a T antigen containing two RB-binding LxCxE motifs. We find that superT-encoding transcripts are abundant in PyV-associated human cancers. Together, we show that comparative transcriptomic approaches can greatly expand known transcript and coding capacity in one of the simplest and most well-studied viral families.
Sample: MCPyV tumor - viral reads; polyA illumina sequencing
SAMN23100641 • SRS11062728 • All experiments • All runs
Library:
Name: MCPyV_J23_253
Instrument: Illumina NovaSeq 6000
Strategy: RNA-Seq
Source: TRANSCRIPTOMIC
Selection: cDNA
Layout: SINGLE
Runs: 1 run, 3,119 spots, 928,256 bases, 389,391b
Run# of Spots# of BasesSizePublished
SRR169368153,119928,256389,391b2022-02-23

ID:
17870040

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