Long-read cDNA sequencing identifies functional pseudogenes in the human transcriptome

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作者
Robin-Lee Troskie
Yohaann Jafrani
Tim R. Mercer
Adam D. Ewing
Geoffrey J. Faulkner
Seth W. Cheetham
机构
[1] Mater Research Institute-University of Queensland,Australian Institute for Bioengineering and Nanotechnology
[2] University of Queensland,Queensland Brain Institute
[3] University of Queensland,undefined
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Pseudogene; PacBio; Long-read; lncRNA; CRISPR;
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摘要
Pseudogenes are gene copies presumed to mainly be functionless relics of evolution due to acquired deleterious mutations or transcriptional silencing. Using deep full-length PacBio cDNA sequencing of normal human tissues and cancer cell lines, we identify here hundreds of novel transcribed pseudogenes expressed in tissue-specific patterns. Some pseudogene transcripts have intact open reading frames and are translated in cultured cells, representing unannotated protein-coding genes. To assess the biological impact of noncoding pseudogenes, we CRISPR-Cas9 delete the nucleus-enriched pseudogene PDCL3P4 and observe hundreds of perturbed genes. This study highlights pseudogenes as a complex and dynamic component of the human transcriptional landscape.
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