Teresa Szczepińska; Katarzyna Kalisiak; Rafal Tomecki; Anna Labno; Lukasz S. Borowski; Tomasz M. Kulinski; Dorota Adamska; Joanna Kosinska; Andrzej Dziembowski

DIS3 shapes the RNA polymerase II transcriptome in humans by degrading a variety of unwanted transcripts

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Figure 5.

DIS3, but not EXOSC10, is involved in snoRNA processing. (A) A genome browser screenshot of the genomic region encompassing SNORD13 snoRNA with mapped RNA-seq and DIS3 PAR-CLIP reads. The uniquely mapped reads are shown for the plus strand. Note that mature snoRNA are underrepresented in the long read RNA-seq libraries. (B) Northern blot analysis of selected snoRNAs, using cell lines with DIS3 and EXOSC10 mutations. Multiple myeloma-associated mutations are represented by 766 and 780 for DIS3 G766R and DIS3 R780G, respectively (Tomecki et al. 2014).

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Published in Advance August 20, 2015, doi: 10.1101/gr.189597.115 Genome Res. 2015. 25: 1622-1633

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DIS3 shapes the RNA polymerase II transcriptome in humans by degrading a variety of unwanted transcripts

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