The impact of chromosomal fusions on 3D genome folding and recombination in the germ line.
Covadonga VaraAndreu Paytuví-GallartYasmina CuarteroLucía Álvarez-GonzálezLaia Marín-GualFrancisca GarciaBeatriu Florit-SabaterLaia CapillaRosa Ana Sanchéz-GuillénSarrate ZaidaRiccardo Aiese CiglianoWalter SanseverinoJeremy B SearleJacint VenturaMarc A Marti-RenomFrançois Le DilyAurora Ruiz-HerreraPublished in: Nature communications (2021)
The spatial folding of chromosomes inside the nucleus has regulatory effects on gene expression, yet the impact of genome reshuffling on this organization remains unclear. Here, we take advantage of chromosome conformation capture in combination with single-nucleotide polymorphism (SNP) genotyping and analysis of crossover events to study how the higher-order chromatin organization and recombination landscapes are affected by chromosomal fusions in the mammalian germ line. We demonstrate that chromosomal fusions alter the nuclear architecture during meiosis, including an increased rate of heterologous interactions in primary spermatocytes, and alterations in both chromosome synapsis and axis length. These disturbances in topology were associated with changes in genomic landscapes of recombination, resulting in detectable genomic footprints. Overall, we show that chromosomal fusions impact the dynamic genome topology of germ cells in two ways: (i) altering chromosomal nuclear occupancy and synapsis, and (ii) reshaping landscapes of recombination.
Keyphrases
- copy number
- genome wide
- dna methylation
- dna damage
- gene expression
- dna repair
- molecular dynamics simulations
- single molecule
- transcription factor
- induced apoptosis
- randomized controlled trial
- cell proliferation
- oxidative stress
- double blind
- cell cycle arrest
- open label
- high throughput
- placebo controlled
- study protocol