Diverse monogenic subforms of human spermatogenic failure

Liina Nagirnaja, Alexandra M. Lopes, Wu Lin Charng, Brian Miller, Rytis Stakaitis, Ieva Golubickaite, Alexandra Stendahl, Tianpengcheng Luan, Corinna Friedrich, Eisa Mahyari, Eloise Fadial, Laura Kasak, Katinka Vigh-Conrad, Manon S. Oud, Miguel J. Xavier, Samuel R. Cheers, Emma R. James, Jingtao Guo, Timothy G. Jenkins, Antoni Riera-EscamillaAlberto Barros, Filipa Carvalho, Susana Fernandes, João Gonçalves, Christina A. Gurnett, Niels Jørgensen, Davor Jezek, Emily S. Jungheim, Sabine Kliesch, Robert I. McLachlan, Kenan R. Omurtag, Adrian Pilatz, Jay I. Sandlow, James Smith, Michael L. Eisenberg, James M. Hotaling, Keith A. Jarvi, Margus Punab, Ewa Rajpert-De Meyts, Douglas T. Carrell, Csilla Krausz, Maris Laan, Moira K. O’Bryan, Peter N. Schlegel, Frank Tüttelmann, Joris A. Veltman, Kristian Almstrup, Kenneth I. Aston, Donald F. Conrad*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

29 Scopus citations

Abstract

Non-obstructive azoospermia (NOA) is the most severe form of male infertility and typically incurable. Defining the genetic basis of NOA has proven challenging, and the most advanced classification of NOA subforms is not based on genetics, but simple description of testis histology. In this study, we exome-sequenced over 1000 clinically diagnosed NOA cases and identified a plausible recessive Mendelian cause in 20%. We find further support for 21 genes in a 2-stage burden test with 2072 cases and 11,587 fertile controls. The disrupted genes are primarily on the autosomes, enriched for undescribed human “knockouts”, and, for the most part, have yet to be linked to a Mendelian trait. Integration with single-cell RNA sequencing data shows that azoospermia genes can be grouped into molecular subforms with synchronized expression patterns, and analogs of these subforms exist in mice. This analysis framework identifies groups of genes with known roles in spermatogenesis but also reveals unrecognized subforms, such as a set of genes expressed across mitotic divisions of differentiating spermatogonia. Our findings highlight NOA as an understudied Mendelian disorder and provide a conceptual structure for organizing the complex genetics of male infertility, which may provide a rational basis for disease classification.

Original languageEnglish (US)
Article number7953
JournalNature communications
Volume13
Issue number1
DOIs
StatePublished - Dec 2022

Funding

We thank all of the study participants and the numerous medical staff that enabled this study. We also acknowledge the contribution of the Lisbon clinical team - Carlos Calhaz-Jorge, Ana Aguiar, Joaquim Nunes, and Sandra Sousa (Unidade de Medicina da Reproducão, Hospital de Santa Maria, Centro Hospitalar Lisboa Norte, Lisboa, Portugal), Maria Graça Pinto and Sónia Correia (Centro de Medicina Reprodutiva), for patients' clinical evaluation.The study has been funded by the following resources. National Institutes of Health of the United States of America grant R01HD078641 (D.F.C, K.I.A) National Institutes of Health of the United States of America grant P50HD096723 (D.F.C.) National Health and Medical Research Council of Australia grant APP1120356 (M.O., D.C., K.I.A., R.M., and J.A.V.) Spanish Ministry of Health Instituto Carlos III-FIS grant FIS/FEDER- PI20/01562 (C.K., A.R.-E.). Estonian Research Council grants IUT34-12 and PRG1021 (M.L., M.P.) ReproUnion and the Innovation Fund Denmark grant 14-2013-4 (K.A.) German Research Foundation Clinical Research Unit ‘Male Germ Cells’ grant DFG CRU326 (C.F., F.T.) The Netherlands Organization for Scientific Research VICI grant 918-15-667 (J.A.V.) Investigator Award in Science from the Wellcome Trust grant 209451 (J.A.V.). FCT/MCTES, through national funds attributed to Centre for Toxicogenomics and Human Health—ToxOmics, grant UID/BIM/00009/2016 (J.Go.) National Institute of Mental Health of the National Institutes of Health grant T32-MH014677 (W.-L.C). We thank all of the study participants and the numerous medical staff that enabled this study. We also acknowledge the contribution of the Lisbon clinical team - Carlos Calhaz-Jorge, Ana Aguiar, Joaquim Nunes, and Sandra Sousa (Unidade de Medicina da Reproducão, Hospital de Santa Maria, Centro Hospitalar Lisboa Norte, Lisboa, Portugal), Maria Graça Pinto and Sónia Correia (Centro de Medicina Reprodutiva), for patients' clinical evaluation.The study has been funded by the following resources. National Institutes of Health of the United States of America grant R01HD078641 (D.F.C, K.I.A) National Institutes of Health of the United States of America grant P50HD096723 (D.F.C.) National Health and Medical Research Council of Australia grant APP1120356 (M.O., D.C., K.I.A., R.M., and J.A.V.) Spanish Ministry of Health Instituto Carlos III-FIS grant FIS/FEDER- PI20/01562 (C.K., A.R.-E.). Estonian Research Council grants IUT34-12 and PRG1021 (M.L., M.P.) ReproUnion and the Innovation Fund Denmark grant 14-2013-4 (K.A.) German Research Foundation Clinical Research Unit ‘Male Germ Cells’ grant DFG CRU326 (C.F., F.T.) The Netherlands Organization for Scientific Research VICI grant 918-15-667 (J.A.V.) Investigator Award in Science from the Wellcome Trust grant 209451 (J.A.V.). FCT/MCTES, through national funds attributed to Centre for Toxicogenomics and Human Health—ToxOmics, grant UID/BIM/00009/2016 (J.Go.) National Institute of Mental Health of the National Institutes of Health grant T32-MH014677 (W.-L.C).

ASJC Scopus subject areas

  • General Chemistry
  • General Biochemistry, Genetics and Molecular Biology
  • General Physics and Astronomy

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