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<i>Prdm9</i> Controls Activation of Mammalian Recombination Hotspots
619
Citations
9
References
2010
Year
GeneticsGenomic MechanismMolecular GeneticsGenomicsReproductive BiologyEpigeneticsTranscriptional RegulationEarly MeiosisGerm Cell FateMeiosisMammalian Meiotic RecombinationChromosomal RearrangementGene ExpressionCell BiologyDevelopmental BiologyZinc FingerChromosome BiologyRecombination DynamicMedicineMammalian Recombination Hotspots
Mammalian meiotic recombination, which preferentially occurs at specialized sites called hotspots, ensures the orderly segregation of meiotic chromosomes and creates genetic variation among offspring. A locus on mouse chromosome 17, which controls activation of recombination at multiple distant hotspots, has been mapped within a 181-kilobase interval, three of whose genes can be eliminated as candidates. The remaining gene, Prdm9, codes for a zinc finger containing histone H3K4 trimethylase that is expressed in early meiosis and whose deficiency results in sterility in both sexes. Mus musculus exhibits five alleles of Prdm9; human populations exhibit two predominant alleles and multiple minor alleles. The identification of Prdm9 as a protein regulating mammalian recombination hotspots initiates molecular studies of this important biological control system.
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