RNF212 is a dosage-sensitive regulator of crossing-over during mammalian meiosis
RNF212 is a dosage-sensitive regulator of crossing-over during mammalian meiosis
Crossing-over ensures accurate chromosome segregation during meiosis, and every pair of chromosomes obtains at least one crossover, even though the majority of recombination sites yield non-crossovers. A putative regulator of crossing-over is RNF212, which is associated with variation in crossover rates in humans. We show that mouse RNF212 is essential for crossing-over, functioning to couple chromosome synapsis to the formation of crossover-specific recombination complexes. Selective localization of RNF212 to a subset of recombination sites is shown to be a key early step in the crossover designation process. RNF212 acts at these sites to stabilize meiosis-specific recombination factors, including the MutSγ complex (MSH4-MSH5). We infer that selective stabilization of key recombination proteins is a fundamental feature of meiotic crossover control. Haploinsufficiency indicates that RNF212 is a limiting factor for crossover control and raises the possibility that human alleles may alter the amount or stability of RNF212 and be risk factors for aneuploid conditions.
- University of Pennsylvania United States
- French National Centre for Scientific Research France
- University of California, Davis United States
- Cornell University United States
- Institute of Human Genetics France
Recombination, Genetic, Ubiquitin-Protein Ligases, Cell Cycle Proteins, Aneuploidy, DNA-Binding Proteins, Ligases, Meiosis, Mice, Chromosome Segregation, Dosage Compensation, Genetic, Animals, Humans, Crossing Over, Genetic
Recombination, Genetic, Ubiquitin-Protein Ligases, Cell Cycle Proteins, Aneuploidy, DNA-Binding Proteins, Ligases, Meiosis, Mice, Chromosome Segregation, Dosage Compensation, Genetic, Animals, Humans, Crossing Over, Genetic
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