Transmission ratio distortion of mutations in the master regulator of centriole biogenesis PLK4

Author:

Neitzel Heidemarie,Varon Raymonda,Chughtai Sana,Dartsch Josephine,Dutrannoy-Tönsing Véronique,Nürnberg Peter,Nürnberg Gudrun,Schweiger Michal,Digweed Martin,Hildebrand Gabriele,Hackmann Karl,Holtgrewe Manuel,Sarioglu Nanette,Schulze Bernt,Horn Denise,Sperling KarlORCID

Abstract

AbstractThe evolutionary conserved Polo-like kinase 4 (PLK4) is essential for centriole duplication, spindle assembly, and de novo centriole formation. In man, homozygous mutations in PLK4 lead to primary microcephaly, altered PLK4 expression is associated with aneuploidy in human embryos. Here, we report on a consanguineous four-generation family with 8 affected individuals compound heterozygous for a novel missense variant, c.881 T > G, and a deletion of the PLK4 gene. The clinical phenotype of the adult patients is mild compared to individuals with previously described PLK4 mutations. One individual was homozygous for the variant c.881G and phenotypically unaffected. The deletion was inherited by 14 of 16 offspring and thus exhibits transmission ratio distortion (TRD). Moreover, based on the already published families with PLK4 mutations, it could be shown that due to the preferential transmission of the mutant alleles, the number of affected offspring is significantly increased. It is assumed that reduced expression of PLK4 decreases the intrinsically high error rate of the first cell divisions after fertilization, increases the number of viable embryos and thus leads to preferential transmission of the deleted/mutated alleles.

Funder

Higher Education Commision, Pakistan

Deutsche Forschungsgemeinschaft

Charité - Universitätsmedizin Berlin

Publisher

Springer Science and Business Media LLC

Subject

Genetics (clinical),Genetics

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