Distinct Classes of Complex Structural Variation Uncovered across Thousands of Cancer Genome Graphs | Zendy

Kevin Hadi | Zendy; Xiaotong Yao | Zendy; Julie M. Behr | Zendy; Aditya Deshpande | Zendy; Charalampos Xanthopoulakis | Zendy; Huasong Tian | Zendy; Sarah Kudman | Zendy; Joel Rosiene | Zendy; Madison Darmofal | Zendy; Joseph DeRose | Zendy; Rick Mortensen | Zendy; Emily M. Adney | Zendy; Alon Shaiber | Zendy; Zoran Gajic | Zendy; Michael Sigouros | Zendy; Kenneth Eng | Zendy; Jeremiah A. Wala | Zendy; Kazimierz O. Wrzeszczyński | Zendy; Kanika Arora | Zendy; Minita Shah | Zendy; Anne-Katrin Emde | Zendy; Vanessa Felice | Zendy; Mayu O. Frank | Zendy; Robert B. Darnell | Zendy; Mahmoud Ghandi | Zendy; Franklin W. Huang | Zendy; Sally M. Dewhurst | Zendy; John Maciejowski | Zendy; Titia de Lange | Zendy; Jeremy Setton | Zendy; Nadeem Riaz | Zendy; Jorge S. ReisFilho | Zendy; Simon N. Powell | Zendy; David A. Knowles | Zendy; Ed Reznik | Zendy; Bud Mishra | Zendy; Rameen Beroukhim | Zendy; Michael C. Zody | Zendy; Nicolas Robine | Zendy; Kenji Oman | Zendy; Carissa A. Sanchez | Zendy; Mary K. Kuhner | Zendy; Lucian P. Smith | Zendy; Patricia C. Galipeau | Zendy; Thomas G. Paulson | Zendy; Brian J. Reid | Zendy; Xiaohong Li | Zendy; David Wilkes | Zendy; Andrea Sboner | Zendy; Juan Miguel Mosquera | Zendy; Olivier Elemento | Zendy; Marcin Imieliński | Zendy

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Distinct Classes of Complex Structural Variation Uncovered across Thousands of Cancer Genome Graphs

Author(s) -

Kevin Hadi,

Xiaotong Yao,

Julie M. Behr,

Aditya Deshpande,

Charalampos Xanthopoulakis,

Huasong Tian,

Sarah Kudman,

Joel Rosiene,

Madison Darmofal,

Joseph DeRose,

Rick Mortensen,

Emily M. Adney,

Alon Shaiber,

Zoran Gajic,

Michael Sigouros,

Kenneth Eng,

Jeremiah A. Wala,

Kazimierz O. Wrzeszczyński,

Kanika Arora,

Minita Shah,

Anne-Katrin Emde,

Vanessa Felice,

Mayu O. Frank,

Robert B. Darnell,

Mahmoud Ghandi,

Franklin W. Huang,

Sally M. Dewhurst,

John Maciejowski,

Titia de Lange,

Jeremy Setton,

Nadeem Riaz,

Jorge S. ReisFilho,

Simon N. Powell,

David A. Knowles,

Ed Reznik,

Bud Mishra,

Rameen Beroukhim,

Michael C. Zody,

Nicolas Robine,

Kenji Oman,

Carissa A. Sanchez,

Mary K. Kuhner,

Lucian P. Smith,

Patricia C. Galipeau,

Thomas G. Paulson,

Brian J. Reid,

Xiaohong Li,

David Wilkes,

Andrea Sboner,

Juan Miguel Mosquera,

Olivier Elemento,

Marcin Imieliński

Publication year - 2020

Publication title -

cell

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 26.304

H-Index - 776

eISSN - 1097-4172

pISSN - 0092-8674

DOI - 10.1016/j.cell.2020.08.006

Subject(s) - biology , chromothripsis , genome , somatic hypermutation , genetics , computational biology , gene , dna , evolutionary biology , dna damage , genome instability , b cell , antibody

Cancer genomes often harbor hundreds of somatic DNA rearrangement junctions, many of which cannot be easily classified into simple (e.g., deletion) or complex (e.g., chromothripsis) structural variant classes. Applying a novel genome graph computational paradigm to analyze the topology of junction copy number (JCN) across 2,778 tumor whole-genome sequences, we uncovered three novel complex rearrangement phenomena: pyrgo, rigma, and tyfonas. Pyrgo are "towers" of low-JCN duplications associated with early-replicating regions, superenhancers, and breast or ovarian cancers. Rigma comprise "chasms" of low-JCN deletions enriched in late-replicating fragile sites and gastrointestinal carcinomas. Tyfonas are "typhoons" of high-JCN junctions and fold-back inversions associated with expressed protein-coding fusions, breakend hypermutation, and acral, but not cutaneous, melanomas. Clustering of tumors according to genome graph-derived features identified subgroups associated with DNA repair defects and poor prognosis.

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