Variant in the synaptonemal complex protein SYCE2 associates with pregnancy loss through effect on recombination

Author:

Steinthorsdottir ValgerdurORCID,Halldorsson Bjarni V.ORCID,Jonsson HakonORCID,Palsson GunnarORCID,Oddsson AsmundurORCID,Westergaard DavidORCID,Arnadottir Gudny A.ORCID,Stefansdottir Lilja,Banasik KarinaORCID,Esplin M. Sean,Hansen Thomas FolkmannORCID,Brunak SørenORCID,Nyegaard MetteORCID,Ostrowski Sisse RyeORCID,Pedersen Ole Birger VesteragerORCID,Erikstrup ChristianORCID,Thorleifsson GudmarORCID,Nadauld Lincoln D.,Haraldsson AsgeirORCID,Steingrimsdottir Thora,Tryggvadottir LaufeyORCID,Jonsdottir IngileifORCID,Gudbjartsson Daniel F.ORCID,Hoffmann Eva R.ORCID,Sulem PatrickORCID,Holm HilmaORCID,Nielsen Henriette SvarreORCID,Stefansson KariORCID,

Abstract

AbstractTwo-thirds of all human conceptions are lost, in most cases before clinical detection. The lack of detailed understanding of the causes of pregnancy losses constrains focused counseling for future pregnancies. We have previously shown that a missense variant in synaptonemal complex central element protein 2 (SYCE2), in a key residue for the assembly of the synaptonemal complex backbone, associates with recombination traits. Here we show that it also increases risk of pregnancy loss in a genome-wide association analysis on 114,761 women with reported pregnancy loss. We further show that the variant associates with more random placement of crossovers and lower recombination rate in longer chromosomes but higher in the shorter ones. These results support the hypothesis that some pregnancy losses are due to failures in recombination. They further demonstrate that variants with a substantial effect on the quality of recombination can be maintained in the population.

Publisher

Springer Science and Business Media LLC

Subject

Molecular Biology,Structural Biology

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