Nature Search

Benchmarking scRNA-seq copy number variation callers

Several computational tools have now been developed to identify copy number variations (CNVs) from scRNA-seq data. Here authors benchmark these methods, showing that performance is affected by dataset quality, CNV type and reference dataset, with methods including allelic information being more robust in large datasets.

Katharina T. Schmid
Aikaterini Symeonidi
Maria Colomé-Tatché
ResearchOpen Access02 Oct 2025
Nature Communications

Volume: 16, P: 1-17
DNA methylation influences human centromere positioning and function

Genome-wide and targeted perturbation of DNA methylation at centromeres affects CENP-A positioning and centromere structure, resulting in aneuploidy and reduced cell viability.

Catalina Salinas-Luypaert
Danilo Dubocanin
Daniele Fachinetti
ResearchOpen Access04 Sept 2025
Nature Genetics

P: 1-13
A compendium of Amplification-Related Gain Of Sensitivity genes in human cancer

In cancer, the impact on cellular fitness of copy-number gains affecting collaterally-amplified genes remains poorly understood compared to oncogenes. Here, the authors integrate genomic data from tumours and cell lines and identify a class of ‘Amplification-Related Gain Of Sensitivity’ (ARGOS) genes, with potential therapeutic applications.

Veronica Rendo
Michael Schubert
Floris Foijer
ResearchOpen Access27 Jan 2025
Nature Communications

Volume: 16, P: 1-18
IL-6R expression is an independent prognostic factor in high-grade serous ovarian cancer

Alexis M. Maagdenberg
Annegé Vledder
Marco de Bruyn
ResearchOpen Access08 Jul 2025
BJC Reports

Volume: 3, P: 1-8
Author Correction: Genetic instability from a single S phase after whole-genome duplication

Simon Gemble
René Wardenaar
Renata Basto
Amendments and CorrectionsOpen Access21 Jul 2022
Nature

Volume: 608, P: E27
Neoadjuvant immune checkpoint blockade in women with mismatch repair deficient endometrial cancer: a phase I study

Immune checkpoint blockade (ICB) has shown promising activity in patients with advanced endometrial cancer, however its potential in the context of loco-regional disease remains unclear. Here the authors report the results of a phase I trial of neoadjuvant pembrolizumab (anti-PD1) in patients with mismatch repair deficient resectable endometrial cancer.

Anneke L. Eerkens
Koen Brummel
Hans W. Nijman
ResearchOpen Access03 Sept 2024
Nature Communications

Volume: 15, P: 1-17
cGAS–STING drives the IL-6-dependent survival of chromosomally instable cancers

The survival of cells with chromosomal instability (CIN) depends on the cGAS–STING pathway, in which IL-6 and its receptor have a key role; this vulnerability can be exploited to treat tumours that display CIN.

Christy Hong
Michael Schubert
Floris Foijer
Research15 Jun 2022
Nature

Volume: 607, P: 366-373
Neurodegeneration-associated protein VAPB regulates proliferation in medulloblastoma

Amanda Faria Assoni
Thiago Giove Mitsugi
Oswaldo Keith Okamoto
ResearchOpen Access09 Nov 2023
Scientific Reports

Volume: 13, P: 1-13
Early evolutionary branching across spatial domains predisposes to clonal replacement under chemotherapy in neuroblastoma

Neuroblastoma (NB) is a frequent childhood cancer that often becomes resistant to therapy. Here, the authors perform spatiotemporal genomic profiling of NBs before and after chemotherapy and find an evolutionary process characteristic of NBs growing resistant after first responding to treatment.

Jenny Karlsson
Hiroaki Yasui
David Gisselsson
ResearchOpen Access18 Oct 2024
Nature Communications

Volume: 15, P: 1-19
Single-cell chromosome and bulk transcriptome analysis as a diagnostic tool to differentiate between localized and metastatic pheochromocytoma and sympathetic paraganglioma

Annika M. A. Berends
René Wardenaar
Floris Foijer
Research03 May 2025
Oncogene

Volume: 44, P: 2547-2560
Acute systemic loss of Mad2 leads to intestinal atrophy in adult mice

Klaske M. Schukken
Yinan Zhu
Floris Foijer
ResearchOpen Access08 Jan 2021
Scientific Reports

Volume: 11, P: 1-8
Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling

Mixed responses to targeted therapy within a patient are a clinical challenge. Here the authors show that TP53 loss-of-function cooperates with whole genome doubling which increases chromosomal instability. This leads to greater cellular diversity and multiple routes of resistance, which in turn promotes mixed responses to treatment.

Sebastijan Hobor
Maise Al Bakir
Charles Swanton
ResearchOpen Access13 Jun 2024
Nature Communications

Volume: 15, P: 1-21
Nuclear chromosome locations dictate segregation error frequencies

Using single-cell DNA sequencing after an error-prone mitosis in untransformed, diploid cell lines and organoids, chromosomes are shown to have different segregation error frequencies that result in non-random aneuploidy landscapes.

Sjoerd J. Klaasen
My Anh Truong
Geert J. P. L. Kops
ResearchOpen Access13 Jul 2022
Nature

Volume: 607, P: 604-609
Clonal origin and development of high hyperdiploidy in childhood acute lymphoblastic leukaemia

High hyperdiploid acute lymphoblastic leukaemia (HeH ALL) is driven by nonrandom chromosomal gains, which have been suggested to arise early - even before birth. Here, the authors use single-cell whole genome sequencing and in silico modelling to show that HeH ALL aneuploidies could originate early and follow punctuated evolution.

Eleanor L. Woodward
Minjun Yang
Kajsa Paulsson
ResearchOpen Access25 Mar 2023
Nature Communications

Volume: 14, P: 1-14
Genetic instability from a single S phase after whole-genome duplication

Extensive DNA damage occurs during the first interphase following induction of tetraploidy in human cells, largely as a result of the lower amount of protein relative to DNA.

Simon Gemble
René Wardenaar
Renata Basto
ResearchOpen Access30 Mar 2022
Nature

Volume: 604, P: 146-151
Aneuploidy renders cancer cells vulnerable to mitotic checkpoint inhibition

Aneuploid cancer cell lines show increased dependence on the spindle assembly complex (SAC); initially they are resistant to SAC perturbations, but over time they accumulate chromosomal aberrations that impair their fitness.

Yael Cohen-Sharir
James M. McFarland
Uri Ben-David
Research27 Jan 2021
Nature

Volume: 590, P: 486-491
A living biobank of ovarian cancer ex vivo models reveals profound mitotic heterogeneity

High-grade serous ovarian carcinoma is often associated with TP53 mutation and chromosomal instability (CIN). Here, the authors generate ex vivo cultures from biopsies and ascites of patients and perform characterization to evaluate CIN mechanisms and compare drug sensitivity with patient responses.

Louisa Nelson
Anthony Tighe
Stephen S. Taylor
ResearchOpen Access13 Feb 2020
Nature Communications

Volume: 11, P: 1-18
Ongoing chromosomal instability and karyotype evolution in human colorectal cancer organoids

The authors use three-dimensional live-cell imaging of colorectal carcinoma organoids to show that chromosomal instability is widespread. Single-cell sequencing identifies heterogeneity of copy number alterations and shows clonal evolution.

Ana C. F. Bolhaqueiro
Bas Ponsioen
Geert J. P. L. Kops
Research29 Apr 2019
Nature Genetics

Volume: 51, P: 824-834
Short-term molecular consequences of chromosome mis-segregation for genome stability

Chromosomal instability leads to aneuploidy, a state of karyotype imbalance. By inducing controlled chromosome mis-segregation, Santaguida and colleagues show that aneuploidy can also instigate chromosomal instability.

Lorenza Garribba
Giuseppina De Feudis
Stefano Santaguida
ResearchOpen Access11 Mar 2023
Nature Communications

Volume: 14, P: 1-17
Progression through mitosis promotes PARP inhibitor-induced cytotoxicity in homologous recombination-deficient cancer cells

Mutations in BRCA1 and BRCA2 render a cancer cell hypersensitive to PARP inhibitors but they can acquire resistance and relapse. Here the authors find that PARP inhibition leads to replication fork instability, cytokinesis failure and cell death, aiding our understanding of how inhibition leads to cytotoxic outcomes.

Pepijn M. Schoonen
Francien Talens
Marcel A. T. M. van Vugt
ResearchOpen Access17 Jul 2017
Nature Communications

Volume: 8, P: 1-13
FoxM1 repression during human aging leads to mitotic decline and aneuploidy-driven full senescence

Evidence for mitotic decline in aged cells and for aneuploidy-driven progression into full senescence is limited. Here, the authors find that in aged cells, mitotic gene repression leads to increased chromosome mis-segregation and aneuploidy that triggers permanent cell cycle arrest and full senescence.

Joana Catarina Macedo
Sara Vaz
Elsa Logarinho
ResearchOpen Access19 Jul 2018
Nature Communications

Volume: 9, P: 1-17
CDK4 is co-amplified with either TP53 promoter gene fusions or MDM2 through distinct mechanisms in osteosarcoma

Karim H. Saba
Valeria Difilippo
Karolin H. Nord
ResearchOpen Access25 Sept 2024
npj Genomic Medicine

Volume: 9, P: 1-12
MDM2 amplification in rod-shaped chromosomes provides clues to early stages of circularized gene amplification in liposarcoma

Amplification in liposarcoma develops through a stepwise process that does not fit with classical chromothripsis. Depending on if and when telomeres from other chromosomes are captured, circularized or linear gain of 12q sequences will predominate.

Saskia Sydow
Paul Piccinelli
Fredrik Mertens
ResearchOpen Access20 May 2024
Communications Biology

Volume: 7, P: 1-12
TPX2/Aurora kinase A signaling as a potential therapeutic target in genomically unstable cancer cells

Stephanie E. van Gijn
Elles Wierenga
Rudolf S. N. Fehrmann
ResearchOpen Access03 Sept 2018
Oncogene

Volume: 38, P: 852-867

Search

Benchmarking scRNA-seq copy number variation callers

DNA methylation influences human centromere positioning and function

A compendium of Amplification-Related Gain Of Sensitivity genes in human cancer

IL-6R expression is an independent prognostic factor in high-grade serous ovarian cancer

Author Correction: Genetic instability from a single S phase after whole-genome duplication

Neoadjuvant immune checkpoint blockade in women with mismatch repair deficient endometrial cancer: a phase I study

cGAS–STING drives the IL-6-dependent survival of chromosomally instable cancers

Neurodegeneration-associated protein VAPB regulates proliferation in medulloblastoma

Early evolutionary branching across spatial domains predisposes to clonal replacement under chemotherapy in neuroblastoma

Single-cell chromosome and bulk transcriptome analysis as a diagnostic tool to differentiate between localized and metastatic pheochromocytoma and sympathetic paraganglioma

Acute systemic loss of Mad2 leads to intestinal atrophy in adult mice

Mixed responses to targeted therapy driven by chromosomal instability through p53 dysfunction and genome doubling

Nuclear chromosome locations dictate segregation error frequencies

Clonal origin and development of high hyperdiploidy in childhood acute lymphoblastic leukaemia

Genetic instability from a single S phase after whole-genome duplication

Aneuploidy renders cancer cells vulnerable to mitotic checkpoint inhibition

A living biobank of ovarian cancer ex vivo models reveals profound mitotic heterogeneity

Ongoing chromosomal instability and karyotype evolution in human colorectal cancer organoids

Short-term molecular consequences of chromosome mis-segregation for genome stability

Progression through mitosis promotes PARP inhibitor-induced cytotoxicity in homologous recombination-deficient cancer cells

FoxM1 repression during human aging leads to mitotic decline and aneuploidy-driven full senescence

CDK4 is co-amplified with either TP53 promoter gene fusions or MDM2 through distinct mechanisms in osteosarcoma

MDM2 amplification in rod-shaped chromosomes provides clues to early stages of circularized gene amplification in liposarcoma

TPX2/Aurora kinase A signaling as a potential therapeutic target in genomically unstable cancer cells

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