The APOBEC3A deaminase drives episodic mutagenesis in cancer cells

Petljak, Mia; Chu, Kevan; Dananberg, Alexandra; Bergstrom, Erik N.; Morgen, Patrick von; Alexandrov, Ludmil B.; Stratton, Michael R.; Maciejowski, John

doi:10.1101/2021.02.14.431145

Cited by 11 publications

(20 citation statements)

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“…By contrast, MBSs have not been comprehensively investigated, presumably owing to their small numbers in cancer genomes. Moreover, only a handful of processes have been associated with omikli and kataegic events, with most processes attributed to the AID and APOBEC3 family Article of deaminases 3,[6][7][8]13,14,[20][21][22][23] . Specifically, the APOBEC3 enzymes, which are typically responsible for antiviral responses [24][25][26][27][28][29][30] , give rise to omikli and kataegis by requiring single-stranded DNA as a substrate 6,8,23,31 .…”

Section: Mapping Clustered Mutations In Cancer Reveals Apobec3 Mutage...mentioning

confidence: 99%

“…Moreover, only a handful of processes have been associated with omikli and kataegic events, with most processes attributed to the AID and APOBEC3 family Article of deaminases 3,[6][7][8]13,14,[20][21][22][23] . Specifically, the APOBEC3 enzymes, which are typically responsible for antiviral responses [24][25][26][27][28][29][30] , give rise to omikli and kataegis by requiring single-stranded DNA as a substrate 6,8,23,31 . Omikli were found to be enriched in early replicating regions and more prevalent in microsatellite stable tumours, indicating that mismatch repair has a role in exposing short single-stranded DNA regions 6 .…”

Section: Mapping Clustered Mutations In Cancer Reveals Apobec3 Mutage...mentioning

confidence: 99%

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Mapping clustered mutations in cancer reveals APOBEC3 mutagenesis of ecDNA

Bergstrom

Luebeck

Petljak

et al. 2022

Nature

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Clustered somatic mutations are common in cancer genomes and previous analyses reveal several types of clustered single-base substitutions, which include doublet- and multi-base substitutions1–5, diffuse hypermutation termed omikli6, and longer strand-coordinated events termed kataegis3,7–9. Here we provide a comprehensive characterization of clustered substitutions and clustered small insertions and deletions (indels) across 2,583 whole-genome-sequenced cancers from 30 types of cancer10. Clustered mutations were highly enriched in driver genes and associated with differential gene expression and changes in overall survival. Several distinct mutational processes gave rise to clustered indels, including signatures that were enriched in tobacco smokers and homologous-recombination-deficient cancers. Doublet-base substitutions were caused by at least 12 mutational processes, whereas most multi-base substitutions were generated by either tobacco smoking or exposure to ultraviolet light. Omikli events, which have previously been attributed to APOBEC3 activity6, accounted for a large proportion of clustered substitutions; however, only 16.2% of omikli matched APOBEC3 patterns. Kataegis was generated by multiple mutational processes, and 76.1% of all kataegic events exhibited mutational patterns that are associated with the activation-induced deaminase (AID) and APOBEC3 family of deaminases. Co-occurrence of APOBEC3 kataegis and extrachromosomal DNA (ecDNA), termed kyklonas (Greek for cyclone), was found in 31% of samples with ecDNA. Multiple distinct kyklonic events were observed on most mutated ecDNA. ecDNA containing known cancer genes exhibited both positive selection and kyklonic hypermutation. Our results reveal the diversity of clustered mutational processes in human cancer and the role of APOBEC3 in recurrently mutating and fuelling the evolution of ecDNA.

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Section: Mapping Clustered Mutations In Cancer Reveals Apobec3 Mutage...mentioning

confidence: 99%

Section: Mapping Clustered Mutations In Cancer Reveals Apobec3 Mutage...mentioning

confidence: 99%

Mapping clustered mutations in cancer reveals APOBEC3 mutagenesis of ecDNA

Bergstrom

Luebeck

Petljak

et al. 2022

Nature

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“…In cancer genomes, omikli were previously attributed to APOBEC3 mutagenesis 15 with some indirect evidence from experimental models 24,[37][38][39] . Our analysis of sequencing data 40 from the clonally expanded breast cancer cell line BT474 with active APOBEC3 mutagenesis experimentally confirmed the existence of APOBEC3 omikli events (cosine similarity: 0.99; Extended Data Fig.…”

Section: Signatures Of Mutational Processes Giving Rise To Clustered Mutationsmentioning

confidence: 99%

“…In contrast, multi-base substitutions have not been comprehensively explored presumably due to their small numbers in most cancer genomes. Moreover, only a handful of reported processes have been associated with omikli and kataegic events with majority of these processes attributed to AID/APOBEC3 family of deaminases 4,5,12,[14][15][16][21][22][23][24] . For example, in B-cell lymphomas clustered tracks of C>T and C>G mutations at WRCY motifs are the result of direct replication over AID lesions 21 .…”

Section: Introductionmentioning

confidence: 99%

“…In addition to AID, the APOBEC3 enzymes, which are typically responsible for anti-viral responses and for limiting the mobility of mobile elements [25][26][27][28][29][30][31] , are a substantial contributor of clustered mutational events 2,4,12,[14][15][16]24,32 . Specifically, the APOBEC3 enzymes give rise to omikli and kataegis by requiring single-stranded DNA as a substrate 14,15,24,32 . Omikli were found enriched in early replicating regions and more prevalent in microsatellite stable tumors indicating a role of mismatch repair in exposing short single-stranded DNA regions while processing mismatched bases during replication 15 .…”

Section: Introductionmentioning

confidence: 99%

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Comprehensive analysis of clustered mutations in cancer reveals recurrent APOBEC3 mutagenesis of ecDNA

Luebeck

Petljak

et al. 2021

Preprint

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Clustered somatic mutations are common in cancer genomes with prior analyses revealing several types of clustered single-base substitutions, including doublet- and multi-base substitutions, diffuse hypermutation termed omikli, and longer strand-coordinated events termed kataegis. Here, we provide a comprehensive characterization of clustered substitutions and clustered small insertions and deletions (indels) across 2,583 whole-genome sequenced cancers from 30 cancer types. While only 3.7% of substitutions and 0.9% of indels were found to be clustered, they contributed 8.4% and 6.9% of substitution and indel drivers, respectively. Multiple distinct mutational processes gave rise to clustered indels including signatures enriched in tobacco smokers and homologous-recombination deficient cancers. Doublet-base substitutions were caused by at least 12 mutational processes, while the majority of multi-base substitutions were generated by either tobacco smoking or exposure to ultraviolet light. Omikli events, previously attributed to the activity of APOBEC3 deaminases, accounted for a large proportion of clustered substitutions. However, only 16.2% of omikli matched APOBEC3 patterns with experimental validation confirming additional mutational processes giving rise to omikli. Kataegis was generated by multiple mutational processes with 76.1% of all kataegic events exhibiting AID/APOBEC3-associated mutational patterns. Co-occurrence of APOBEC3 kataegis and extrachromosomal-DNA (ecDNA) was observed in 31% of samples with ecDNA. Multiple distinct APOBEC3 kataegic events were observed on most mutated ecDNA. ecDNA containing known cancer genes exhibited both positive selection and kataegic hypermutation. Our results reveal the diversity of clustered mutational processes in human cancer and the role of APOBEC3 in recurrently mutating and fueling the evolution of ecDNA.

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