Innovative all-in-one exome sequencing strategy for diagnostic genetic testing in male infertility: Validation and 10-month experience

Manon S Oud; Nicole de Leeuw; Dominique F C M Smeets; Liliana Ramos; Godfried W van der Heijden; Raoul G J Timmermans; Maartje van de Vorst; Tom Hofste; Marlies J E Kempers; Marijn F Stokman; Kathleen W M D'Hauwers; Brigitte H W Faas; Dineke Westra

doi:10.1111/andr.13742

Innovative all-in-one exome sequencing strategy for diagnostic genetic testing in male infertility: Validation and 10-month experience

Andrology. 2024 Aug 24. doi: 10.1111/andr.13742. Online ahead of print.

Affiliations

¹ Department of Human Genetics, Radboud university medical center, Nijmegen, The Netherlands.
² Department of Obstetrics and Gynaecology, Radboud university medical center, Nijmegen, The Netherlands.
³ Department of Urology, Radboud university medical center, Nijmegen, The Netherlands.

PMID: 39180390
DOI: 10.1111/andr.13742

Abstract

Background: Current guidelines indicate that patients with extreme oligozoospermia or azoospermia should be tested for chromosomal imbalances, azoospermia factor (AZF) deletions and/or CFTR variants. For other sperm abnormalities, no genetic diagnostics are recommended.

Objectives: To determine whether exome sequencing (ES) with combined copy number variant (CNV) and single nucleotide variant (SNV) analysis is a reliable first-tier method to replace current methods (validation study), and to evaluate the diagnostic yield after 10 months of implementation (evaluation study).

Materials and methods: In the validation study, ES was performed on DNA of patients already diagnosed with AZF deletions (n = 17), (non-)mosaic sex chromosomal aneuploidies or structural chromosomal anomalies (n = 37), CFTR variants (n = 26), or variants in known infertility genes (n = 4), and 90 controls. The data were analyzed using our standard diagnostic pipeline, with a bioinformatic filter for 130 male infertility genes. In the evaluation study, results of 292 clinical exomes were included.

Results: All previously reported variants in the validation cohort, including clinically relevant Y-chromosomal microdeletions, were correctly identified and reliably detected. In the evaluation study, we identified one or more clinically relevant genetic anomalies in 67 of 292 of all cases (22.9%): these included aberrations that could have been detected with current methods in 30 of 67 patients (10.2% of total), (possible) (mono)genetic causes in the male infertility gene panel in 28 of 67 patients (9.6%), and carriership of cystic fibrosis in nine of 67 patients (3.1%).

Conclusion: ES is a reliable first-tier method to detect the most common genetic causes of male infertility and, as additional genetic causes can be detected, in our evaluation cohort the diagnostic yield almost doubled (10.2%-19.8%, excluding CF carriers). A genetic diagnosis provides answers on the cause of infertility and helps the professionals in the counseling for treatment, possible co-morbidities and risk for offspring and/or family members. Karyotyping will still remain necessary for detecting balanced translocations or low-grade chromosomal mosaicism.

Keywords: asthenozoospermia; azoospermia; diagnostics; gene panel; genetic testing; genetics; male infertility; oligozoospermia; teratozoospermia.