A report of two homozygous TERB1 protein-truncating variants in two unrelated women with primary infertility.

Yalcin Z; Liang M; Abdelrazek IM; Friedrich C; Bareke E; Nabil A; Tüttelmann F; Majewski J; Abdalla E; Tan SL; Slim R

Research article (journal) | Peer reviewed

Abstract

Purpose: To investigate the genetic etiology of patients with female infertility. Methods: Whole Exome Sequencing was performed on genomic DNA extracted from the patient's blood. Exome data were filtered for damaging rare biallelic variants in genes with possible roles in reproduction. Sanger sequencing was used to validate the selected variants and segregate them in family members. Results: A novel homozygous likely pathogenic variant, c.626G>A, p.Trp209*, was identified in the TERB1 gene of the patient. Additionally, we report a second homozygous pathogenic TERB1 variant, c.1703C>G, p.Ser568*, in an infertile woman whose azoospermic brother was previously described to be homozygous for her variant. Conclusions: Here, we report for the first time two homozygous likely pathogenic and pathogenic TERB1 variants, c.626G>A, p.Trp209* and c.1703C>G, p.Ser568*, respectively, in two unrelated women with primary infertility. TERB1 is known to play an essential role in homologous chromosome movement, synapsis, and recombination during the meiotic prophase I and has an established role in male infertility in humans. Our data add TERB1 to the shortlist of Meiosis I genes associated with human infertility in both sexes.

Details about the publication

JournalJournal of Assisted Reproduction and Genetics (J Assist Reprod Genet)
Volume41
Issue3
Page range751-756
StatusPublished
Release year2024 (26/01/2024)
Language in which the publication is writtenEnglish
DOI10.1007/s10815-024-03031-x
KeywordsTERB1; Female infertility; Genetics; Meiosis; Mutation

Authors from the University of Münster

Tüttelmann, Frank
Institute of Human Genetics