Parallel sequencing of extrachromosomal circular DNAs and transcriptomes in single cancer cells

González, Rocío Chamorro; Conrad, Thomas; Stöber, Maja C; Xu, Robin; Giurgiu, Mădălina; Kasack, Katharina; Brückner, Lotte; Rodríguez-Fos, Elias; Helmsauer, Konstantin; García, Heathcliff Dorado; Валиева, М. Е.; Hung, King L.; Bei, Yi; Schmelz, Karin; Lodrini, Marco; Mundlos, Stefan; Chang, Howard Y.; Deubzer, Hedwig E.; Sauer, Sascha; Eggert, Angelika; Schulte, Johannes H.; Schwarz, Roland F.; Haase, Kerstin; Koche, Richard P.; Henssen, Anton

doi:10.1038/s41588-023-01386-y

Cited by 32 publications

(17 citation statements)

References 73 publications

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“…The reconstructed ecDNA elements varied greatly in their complexity (Figure 4f) and ranged from very simple (Figure 4a) or multi-region (Figure 4b) to heavily rearranged complex structures (Figure 4c,d,e). Decoil reconstructs for Patient 4 two ecDNA elements with an individual estimated proportions of more than 700x, resolving the same breakpoints as previously published ([8], Fig. 7a).…”

Section: Resultssupporting

confidence: 78%

“…The reconstructed ecDNA elements varied greatly in their complexity (Figure 4f) and ranged from very simple (Figure 4a) or multi-region (Figure 4b) to heavily rearranged multi-fragmented structures (Figure 4c,d). Decoil reconstructed two ecDNA elements with an individual estimated proportions of more than 700x in patient #4, resolving the same breakpoints as previously described in single cell ecDNA sequencing data from this tumor ( [7]). For samples with a very high structural-variant density at the genomic site of ecDNA origin, Decoil reconstructed multiple circular elements with di↵erent estimated relative proportions, which indicates ecDNA structural heterogeneity (Figure 4e).…”

Section: Exploring Structural Ecdna Complexity In Cancer Patients Usi...mentioning

confidence: 87%

“…Due to their random mitotic segregation, many ecDNA elements, which may structurally differ, co-occur in the same cancer cells [8]. Disentangling ecDNA with shared genomic regions has not yet been addressed by other methods, and it cannot be resolved by de-novo assemblers (e.g.…”

Section: Discussionmentioning

confidence: 99%

“…To assess Decoil's reconstruction performance, we generated an in-silico collection of ecDNA elements, spanning various sequence complexities for systematic evaluation. We introduced a ranking system and defined seven topologies of increasing computational complexity, based on the SV's contained on the ecDNA element: (1) Simple circularization -no structural variants on the ecDNA template, (2) Simple SV's -ecDNA contains either a series of inversions or deletions, (3) Mixed SV's -ecDNA has a combination of inversions and deletions, (4) Multi-region -ecDNA contains di↵erent genomic regions from the same chromosome (DEL, INV and TRA allowed), (5) Multi-chromosomal -ecDNA originates from multiple chromosomes (DEL, INV and TRA allowed), (6) Duplications -ecDNA contains duplications defined as a region larger than 50 bp repeated on the amplicon (DUP's + other simple rearrangements), (7) Foldbacks -ecDNA contains a foldback defined as a two consecutive fragments which overlap in the genomic space, with di↵erent orientations (INVDUP's + all other simple SV's). Every topology can contain a mixture of all other low-rank topologies.…”

Section: Ranking Ecdna Topologies Definitionmentioning

confidence: 99%

“…repeats), which pose a challenge to mapping and de-novo assembly based methods. On the other hand, one tumor can contain different ecDNA elements [7, 8], which can either originate from different or shared genomic locations [9]. The latter scenario may be very challenging for ecDNA reconstruction, as different co-occurring ecDNA elements have overlapping genomic footprints, making it difficult to attribute the overlapping features to each of the different circular elements.…”

Section: Introductionmentioning

confidence: 99%

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Decoil: Reconstructing extrachromosomal DNA structural heterogeneity from long-read sequencing data

Giurgiu,

Wittstruck,

Rodriguez-Fos

et al. 2023

Preprint

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Circular extrachromosomal DNA (ecDNA) is a form of oncogene amplification found across cancer types and associated with poor outcome in patients. ecDNA can be structurally complex and contain rearranged DNA sequences derived from multiple chromosome locations. As the structure of ecDNA can impact oncogene regulation and may indicate mechanisms of its formation, disentangling it at high resolution from sequencing data is essential. Even though methods have been developed to identify and reconstruct ecDNA in cancer genome sequencing, it remains challenging to resolve complex ecDNA structures, in particular amplicons with shared genomic footprints. We here introduce Decoil, a computational method which combines a breakpoint-graph approach withLASSOregression to reconstruct complex ecDNA and deconvolve co-occurring ecDNA elements with overlapping genomic footprints from long-read nanopore sequencing. Decoil outperformsde-novoassembly methods in simulated long-read sequencing data for both, simple and complex ecDNAs. Applying Decoil on whole genome sequencing data uncovered different ecDNA topologies and explored ecDNA structure heterogeneity in neuroblastoma tumors and cell lines, indicating that this method may improve ecDNA structural analyzes in cancer.

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Section: Resultssupporting

confidence: 78%

Section: Exploring Structural Ecdna Complexity In Cancer Patients Usi...mentioning

confidence: 87%

Section: Discussionmentioning

confidence: 99%

Section: Ranking Ecdna Topologies Definitionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Decoil: Reconstructing extrachromosomal DNA structural heterogeneity from long-read sequencing data

Giurgiu,

Wittstruck,

Rodriguez-Fos

et al. 2023

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

Decoil: Reconstructing Extrachromosomal DNA Structural Heterogeneity from Long-Read Sequencing Data

Giurgiu,

Wittstruck,

Rodriguez-Fos

et al. 2024

Lecture Notes in Computer Science

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Imaging extrachromosomal DNA (ecDNA) in cancer

Purshouse,

Pollard,

Bickmore

2024

Histochem Cell Biol

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Extrachromosomal DNA (ecDNA) are circular regions of DNA that are found in many cancers. They are an important means of oncogene amplification, and correlate with treatment resistance and poor prognosis. Consequently, there is great interest in exploring and targeting ecDNA vulnerabilities as potential new therapeutic targets for cancer treatment. However, the biological significance of ecDNA and their associated regulatory control remains unclear. Light microscopy has been a central tool in the identification and characterisation of ecDNA. In this review we describe the different cellular models available to study ecDNA, and the imaging tools used to characterise ecDNA and their regulation. The insights gained from quantitative imaging are discussed in comparison with genome sequencing and computational approaches. We suggest that there is a crucial need for ongoing innovation using imaging if we are to achieve a full understanding of the dynamic regulation and organisation of ecDNA and their role in tumourigenesis.

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Parallel sequencing of extrachromosomal circular DNAs and transcriptomes in single cancer cells

Cited by 32 publications

References 73 publications

Decoil: Reconstructing extrachromosomal DNA structural heterogeneity from long-read sequencing data

Decoil: Reconstructing extrachromosomal DNA structural heterogeneity from long-read sequencing data

Decoil: Reconstructing Extrachromosomal DNA Structural Heterogeneity from Long-Read Sequencing Data

Imaging extrachromosomal DNA (ecDNA) in cancer

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