| Literature DB >> 25486549 |
Henrik Sahlin Pettersen1, Anastasia Galashevskaya2, Berit Doseth2, Mirta M L Sousa3, Antonio Sarno2, Torkild Visnes2, Per Arne Aas2, Nina-Beate Liabakk2, Geir Slupphaug3, Pål Sætrom4, Bodil Kavli5, Hans E Krokan6.
Abstract
The most common mutations in cancer are C to T transitions, but their origin has remained elusive. Recently, mutational signatures of APOBEC-family cytosine deaminases were identified in many common cancers, suggesting off-target deamination of cytosine to uracil as a common mutagenic mechanism. Here we present evidence from mass spectrometric quantitation of deoxyuridine in DNA that shows significantly higher genomic uracil content in B-cell lymphoma cell lines compared to non-lymphoma cancer cell lines and normal circulating lymphocytes. The genomic uracil levels were highly correlated with AID mRNA and protein expression, but not with expression of other APOBECs. Accordingly, AID knockdown significantly reduced genomic uracil content. B-cells stimulated to express endogenous AID and undergo class switch recombination displayed a several-fold increase in total genomic uracil, indicating that B cells may undergo widespread cytosine deamination after stimulation. In line with this, we found that clustered mutations (kataegis) in lymphoma and chronic lymphocytic leukemia predominantly carry AID-hotspot mutational signatures. Moreover, we observed an inverse correlation of genomic uracil with uracil excision activity and expression of the uracil-DNA glycosylases UNG and SMUG1. In conclusion, AID-induced mutagenic U:G mismatches in DNA may be a fundamental and common cause of mutations in B-cell malignancies.Entities:
Keywords: Activation-induced cytidine deaminase (AID); B-cell lymphoma; Base excision repair; Genomic uracil; Kataegis; Mutational signature
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Year: 2014 PMID: 25486549 DOI: 10.1016/j.dnarep.2014.11.006
Source DB: PubMed Journal: DNA Repair (Amst) ISSN: 1568-7856