Maternal exome analysis for the diagnosis of oocyte maturation defects and early embryonic developmental arrest

Antonio Capalbo; Silvia Buonaiuto; Matteo Figliuzzi; Gianluca Damaggio; Laura Girardi; Silvia Caroselli; Maurizio Poli; Cristina Patassini; Murat Cetinkaya; Beril Yuksel; Ajuna Azad; Marie Louise Grøndahl; Eva R Hoffmann; Carlos Simón; Vincenza Colonna; Semra Kahraman

doi:10.1016/j.rbmo.2022.05.009

Maternal exome analysis for the diagnosis of oocyte maturation defects and early embryonic developmental arrest

Reprod Biomed Online. 2022 Sep;45(3):508-518. doi: 10.1016/j.rbmo.2022.05.009. Epub 2022 May 21.

Authors

Antonio Capalbo¹, Silvia Buonaiuto², Matteo Figliuzzi³, Gianluca Damaggio², Laura Girardi³, Silvia Caroselli³, Maurizio Poli³, Cristina Patassini³, Murat Cetinkaya⁴, Beril Yuksel⁴, Ajuna Azad⁵, Marie Louise Grøndahl⁶, Eva R Hoffmann⁵, Carlos Simón⁷, Vincenza Colonna², Semra Kahraman⁴

Affiliations

¹ Reproductive Genetics, Igenomix, Marostica, Italy; Reproductive Genetics, Igenomix Foundation - INCLIVA, Valencia, Spain. Electronic address: antcapalbo@gmail.com.
² Institute of Genetics and Biophysics, National Research Council, Naples, Italy.
³ Reproductive Genetics, Igenomix, Marostica, Italy.
⁴ Istanbul Memorial Hospital, ART and Reproductive Genetics Center Istanbul, Turkey.
⁵ DNRF Center for Chromosome Stability, Department of Cellular and Molecular Medicine, Faculty of Health and Medical Sciences, University of Copenhagen, Denmark.
⁶ Department of Obstetrics and Gynaecology, Department of Reproductive Medicine, Copenhagen University Hospital Herlev, Denmark.
⁷ Reproductive Genetics, Igenomix Foundation - INCLIVA, Valencia, Spain; Harvard University, Department of Obstetrics and Gynaecology BIDMC, Cambridge MA, USA; Department of Obstetrics and Gynaecology, University of Valencia, Valencia, Spain.

PMID: 35798635
DOI: 10.1016/j.rbmo.2022.05.009

Abstract

Research question: Can a methodology be developed for case selection and whole-exome sequencing (WES) analysis of women who are infertile owing to recurrent oocyte maturation defects (OOMD) and/or preimplantation embryo lethality (PREMBL)?

Design: Data were collected from IVF patients attending the Istanbul Memorial Hospital (2015-2021). A statistical methodology to identify infertile endophenotypes (recurrent low oocyte maturation rate, low fertilization rate and preimplantation developmental arrest) was developed using a large IVF dataset (11,221 couples). Twenty-eight infertile women with OOMD/PREMBL were subsequently enrolled for WES on their genomic DNA. Pathogenic variants were prioritized using a custom-made bioinformatic pipeline set to minimize false-positive discoveries through resampling in control cohorts (the Human Genome Diversity Project and 1343 whole-exome sequences from oocyte donors). Individual single-cell RNA sequencing data from 18 human metaphase II (MII) oocytes and antral granulosa cells was used for genome-wide validation. WES and bioinformatics were performed at Igenomix and the National Research Council, Italy.

Results: Variant prioritization analysis identified 265 unique variants in 248 genes (average 22.4 per sample). Of the genes harbouring high-impact variants 78% were expressed by MII oocytes and/or antral granulosa cells, significantly higher than for random sample of controls (odds ratio = 5, Fisher's exact P = 0.0004). Seven of the 28 women (25%) were homozygous carriers of missense pathogenic variants in known candidate genes for OOMD/PREMBL, including PATL2, NLRP5 (n = 2),TLE6, PADI6, TUBB8 and TRIP13. Furthermore, novel gene-disease associations were identified. In fact, one woman with a low oocyte maturation rate was a homozygous carrier of high-impact variants in ENSA, an essential gene for prophase I meiotic transition in mice.

Conclusions: This analytical framework could reveal known and new genes associated with isolated recurrent OOMD/PREMBL, providing essential indications for scaling this strategy to larger studies.

Keywords: Abnormal fertilization; Embryo development; Exome sequencing; Genetics of infertility; Oocyte maturation.

MeSH terms

ATPases Associated with Diverse Cellular Activities
Animals
Cell Cycle Proteins / genetics
Exome
Exome Sequencing
Female
Humans
Infertility, Female* / genetics
Mice
Oocytes / pathology
Oogenesis
Tubulin / genetics

Substances

Cell Cycle Proteins
TUBB8 protein, human
Tubulin
ATPases Associated with Diverse Cellular Activities
TRIP13 protein, human