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Common variants spanning PLK4 are associated with mitotic-origin aneuploidy in human embryos.


ABSTRACT: Aneuploidy, the inheritance of an atypical chromosome complement, is common in early human development and is the primary cause of pregnancy loss. By screening day-3 embryos during in vitro fertilization cycles, we identified an association between aneuploidy of putative mitotic origin and linked genetic variants on chromosome 4 of maternal genomes. This associated region contains a candidate gene, Polo-like kinase 4 (PLK4), that plays a well-characterized role in centriole duplication and has the ability to alter mitotic fidelity upon minor dysregulation. Mothers with the high-risk genotypes contributed fewer embryos for testing at day 5, suggesting that their embryos are less likely to survive to blastocyst formation. The associated region coincides with a signature of a selective sweep in ancient humans, suggesting that the causal variant was either the target of selection or hitchhiked to substantial frequency.

SUBMITTER: McCoy RC 

PROVIDER: S-EPMC5519344 | biostudies-literature | 2015 Apr

REPOSITORIES: biostudies-literature

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Common variants spanning PLK4 are associated with mitotic-origin aneuploidy in human embryos.

McCoy Rajiv C RC   Demko Zachary Z   Ryan Allison A   Banjevic Milena M   Hill Matthew M   Sigurjonsson Styrmir S   Rabinowitz Matthew M   Fraser Hunter B HB   Petrov Dmitri A DA  

Science (New York, N.Y.) 20150401 6231


Aneuploidy, the inheritance of an atypical chromosome complement, is common in early human development and is the primary cause of pregnancy loss. By screening day-3 embryos during in vitro fertilization cycles, we identified an association between aneuploidy of putative mitotic origin and linked genetic variants on chromosome 4 of maternal genomes. This associated region contains a candidate gene, Polo-like kinase 4 (PLK4), that plays a well-characterized role in centriole duplication and has t  ...[more]

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