Skewed X-Chromosome Inactivation as a Possible Marker of X-Linked CNV in Women with Pregnancy Loss

Author:

Fonova Elizaveta A.ORCID,Tolmacheva Ekaterina N.ORCID,Kashevarova Anna A.,Sazhenova Elena A.,Nikitina Tatyana V.ORCID,Lopatkina Maria E.,Vasilyeva Oksana Yu.,Zarubin Aleksei А.ORCID,Aleksandrova Tatyana N.,Yuriev Sergey Yu.ORCID,Skryabin Nikolay A.,Stepanov Vadim A.,Lebedev Igor N.ORCID

Abstract

Skewed X-chromosome inactivation (sXCI) can be a marker of lethal genetic variants on the X chromosome in a woman since sXCI modifies the pathological phenotype. The aim of this study was to search for CNVs in women with miscarriages and sXCI. XCI was assayed using the classical method based on the amplification of highly polymorphic exon 1 of the androgen receptor (<i>AR</i>) gene. The XCI status was analysed in 313 women with pregnancy loss and in 87 spontaneously aborted embryos with 46,XX karyotype, as well as in control groups of 135 women without pregnancy loss and 64 embryos with 46,XX karyotype from induced abortions in women who terminated a normal pregnancy. The frequency of sXCI differed significantly between women with miscarriages and women without pregnancy losses (6.3% and 2.2%, respectively; <i>p</i> = 0.019). To exclude primary causes of sXCI, sequencing of the <i>XIST</i> and <i>XACT</i> genes was performed. The <i>XIST</i> and <i>XACT</i> gene sequencing revealed no known pathogenic variants that could lead to sXCI. Molecular karyotyping was performed using aCGH, followed by verification of X-linked CNVs by RT-PCR and MLPA. Microdeletions at Xp11.23 and Xq24 as well as gains of Xq28 were detected in women with sXCI and pregnancy loss.

Publisher

S. Karger AG

Subject

Genetics (clinical),Genetics,Molecular Biology

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