C19ORF84 connects piRNA and DNA methylation machineries to defend the mammalian germ line

Ansgar Zoch; Gabriela Konieczny; Tania Auchynnikava; Birgit Stallmeyer; Nadja Rotte; Madeleine Heep; Rebecca V Berrens; Martina Schito; Yuka Kabayama; Theresa Schöpp; Sabine Kliesch; Brendan Houston; Liina Nagirnaja; Moira K O'Bryan; Kenneth I Aston; Donald F Conrad; Juri Rappsilber; Robin C Allshire; Atlanta G Cook; Frank Tüttelmann; Dónal O'Carroll

doi:10.1016/j.molcel.2024.01.014

C19ORF84 connects piRNA and DNA methylation machineries to defend the mammalian germ line

Mol Cell. 2024 Mar 21;84(6):1021-1035.e11. doi: 10.1016/j.molcel.2024.01.014. Epub 2024 Feb 14.

Authors

Ansgar Zoch¹, Gabriela Konieczny², Tania Auchynnikava³, Birgit Stallmeyer⁴, Nadja Rotte⁴, Madeleine Heep², Rebecca V Berrens⁵, Martina Schito², Yuka Kabayama², Theresa Schöpp², Sabine Kliesch⁶, Brendan Houston⁷, Liina Nagirnaja⁸, Moira K O'Bryan⁷, Kenneth I Aston⁹, Donald F Conrad¹⁰, Juri Rappsilber¹¹, Robin C Allshire³, Atlanta G Cook³, Frank Tüttelmann⁴, Dónal O'Carroll¹²

Affiliations

¹ Centre for Regenerative Medicine, Institute for Regeneration and Repair, Institute for Stem Cell Research, University of Edinburgh, 5 Little France Drive, Edinburgh EH16 4UU, UK; Wellcome Centre for Cell Biology, University of Edinburgh, Michael Swann Building, Max Born Crescent, Edinburgh EH9 3BF, UK. Electronic address: ansgar.zoch@ed.ac.uk.
² Centre for Regenerative Medicine, Institute for Regeneration and Repair, Institute for Stem Cell Research, University of Edinburgh, 5 Little France Drive, Edinburgh EH16 4UU, UK; Wellcome Centre for Cell Biology, University of Edinburgh, Michael Swann Building, Max Born Crescent, Edinburgh EH9 3BF, UK.
³ Wellcome Centre for Cell Biology, University of Edinburgh, Michael Swann Building, Max Born Crescent, Edinburgh EH9 3BF, UK.
⁴ Institute of Reproductive Genetics, University of Münster, Münster, Germany.
⁵ Institute for Developmental and Regenerative Medicine, University of Oxford, IMS-Tetsuya Nakamura Building, Old Road Campus, Roosevelt Drive, Oxford OX37TY, UK.
⁶ Centre of Reproductive Medicine and Andrology, Department of Clinical and Surgical Andrology, University Hospital Münster, Münster, Germany.
⁷ School of BioSciences and Bio21 Institute, Faculty of Science, The University of Melbourne, Parkville, VIC, Australia.
⁸ Division of Genetics, Oregon National Primate Research Center, Oregon Health and Science University, Beaverton, OR, USA.
⁹ Andrology and In Vitro Fertilization Laboratory, Department of Surgery (Urology), University of Utah School of Medicine, Salt Lake City, UT, USA.
¹⁰ Division of Genetics, Oregon National Primate Research Center, Oregon Health and Science University, Beaverton, OR, USA; Center for Embryonic Cell and Gene Therapy, Oregon Health and Science University, Portland, OR, USA.
¹¹ Wellcome Centre for Cell Biology, University of Edinburgh, Michael Swann Building, Max Born Crescent, Edinburgh EH9 3BF, UK; Bioanalytics, Institute of Biotechnology, Technische Universität Berlin, Gustav-Meyer-Allee 25, 13355 Berlin, Germany.
¹² Centre for Regenerative Medicine, Institute for Regeneration and Repair, Institute for Stem Cell Research, University of Edinburgh, 5 Little France Drive, Edinburgh EH16 4UU, UK; Wellcome Centre for Cell Biology, University of Edinburgh, Michael Swann Building, Max Born Crescent, Edinburgh EH9 3BF, UK. Electronic address: donal.ocarroll@ed.ac.uk.

PMID: 38359823
PMCID: PMC10960678 (available on 2025-03-21)
DOI: 10.1016/j.molcel.2024.01.014

Abstract

In the male mouse germ line, PIWI-interacting RNAs (piRNAs), bound by the PIWI protein MIWI2 (PIWIL4), guide DNA methylation of young active transposons through SPOCD1. However, the underlying mechanisms of SPOCD1-mediated piRNA-directed transposon methylation and whether this pathway functions to protect the human germ line remain unknown. We identified loss-of-function variants in human SPOCD1 that cause defective transposon silencing and male infertility. Through the analysis of these pathogenic alleles, we discovered that the uncharacterized protein C19ORF84 interacts with SPOCD1. DNMT3C, the DNA methyltransferase responsible for transposon methylation, associates with SPOCD1 and C19ORF84 in fetal gonocytes. Furthermore, C19ORF84 is essential for piRNA-directed DNA methylation and male mouse fertility. Finally, C19ORF84 mediates the in vivo association of SPOCD1 with the de novo methylation machinery. In summary, we have discovered a conserved role for the human piRNA pathway in transposon silencing and C19ORF84, an uncharacterized protein essential for orchestrating piRNA-directed DNA methylation.

Keywords: DNA methylation; DNMT3C; PIWI; germline; human male fertility; piRNA; transposon.

MeSH terms

Animals
Argonaute Proteins / genetics
Argonaute Proteins / metabolism
DNA Methylation*
DNA Transposable Elements / genetics
Germ Cells / metabolism
Humans
Male
Mammals / metabolism
Mice
Piwi-Interacting RNA*
Proteins / metabolism
RNA, Small Interfering / genetics
RNA, Small Interfering / metabolism

Substances

Piwi-Interacting RNA
RNA, Small Interfering
Proteins
Argonaute Proteins
DNA Transposable Elements
PIWIL4 protein, mouse

Abstract

MeSH terms

Substances

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