| Literature DB >> 29671673 |
Annica Hedberg1, Erik Knutsen1, Anne Silje Løvhaugen1, Tor Erik Jørgensen2, Maria Perander1, Steinar D Johansen1,2.
Abstract
Low-level mitochondrial heteroplasmy is a common phenomenon in both normal and cancer cells. Here, we investigate the link between low-level heteroplasmy and mitogenome mutations in a human breast cancer matched cell line by high-throughput sequencing. We identified 23 heteroplasmic sites, of which 15 were common between normal cells (Hs578Bst) and cancer cells (Hs578T). Most sites were clustered within the highly conserved Complex IV and ribosomal RNA genes. Two heteroplasmic variants in normal cells were found as fixed mutations in cancer cells. This indicates a positive selection of these variants in cancer cells. RNA-Seq analysis identified upregulated L-strand specific transcripts in cancer cells, which include three mitochondrial long non-coding RNA molecules. We hypothesize that this is due to two cancer cell-specific mutations in the control region.Entities:
Keywords: Cancer cell; SOLiD sequencing; heteroplasmy; lncRNA; mitogenome; mitotranscriptome
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Year: 2018 PMID: 29671673 DOI: 10.1080/24701394.2018.1461852
Source DB: PubMed Journal: Mitochondrial DNA A DNA Mapp Seq Anal ISSN: 2470-1394 Impact factor: 1.514