ADAD2 functions in spermiogenesis and piRNA biogenesis in mice

Author:

Lu Yonggang12,Nagamori Ippei3,Kobayashi Hisato4,Kojima‐Kita Kanako3,Shirane Kenjiro5,Chang Hsin‐Yi26,Nishimura Toru7,Koyano Takayuki8,Yu Zhifeng9,Castañeda Julio M.2,Matsuyama Makoto8,Kuramochi‐Miyagawa Satomi357,Matzuk Martin M.9ORCID,Ikawa Masahito1261011ORCID

Affiliation:

1. Immunology Frontier Research Center Osaka University Osaka Japan

2. Department of Experimental Genome Research Research Institute for Microbial Diseases Osaka University Osaka Japan

3. Department of Pathology Graduate School of Medicine Osaka University Osaka Japan

4. Department of Embryology Nara Medical University Kashihara Nara Japan

5. Department of Genome Biology Graduate School of Medicine Osaka University Osaka Japan

6. Graduate School of Medicine Osaka University Osaka Japan

7. Graduate School of Frontier Biosciences Osaka University Osaka Japan

8. Division of Molecular Genetics Shigei Medical Research Institute Okayama Japan

9. Center for Drug Discovery and Department of Pathology & Immunology Baylor College of Medicine Houston Texas USA

10. Laboratory of Reproductive Systems Biology Institute of Medical Science The University of Tokyo Tokyo Japan

11. Center for Infectious Disease Education and Research Osaka University Osaka Japan

Abstract

AbstractBackgroundAdenosine deaminase domain containing 2 (ADAD2) is a testis‐specific protein composed of a double‐stranded RNA binding domain and a non‐catalytic adenosine deaminase domain. A recent study showed that ADAD2 is indispensable for the male reproduction in mice. However, the detailed functions of ADAD2 remain elusive.ObjectivesThis study aimed to investigate the cause of male sterility in Adad2 mutant mice and to understand the molecular functions of ADAD2.Materials and methodsAdad2 homozygous mutant mouse lines, Adad2–/– and Adad2Δ/Δ, were generated by CRISPR/Cas9. Western blotting and immunohistochemistry were used to reveal the expression and subcellular localization of ADAD2. Co‐immunoprecipitation tandem mass spectrometry was employed to determine the ADAD2‐interacting proteins in mouse testes. RNA‐sequencing analyses were carried out to analyze the transcriptome and PIWI‐interacting RNA (piRNA) populations in wildtype and Adad2 mutant testes.ResultsAdad2–/– and Adad2Δ/Δ mice exhibit male‐specific sterility because of abnormal spermiogenesis. ADAD2 interacts with multiple RNA‐binding proteins involved in piRNA biogenesis, including MILI, MIWI, RNF17, and YTHDC2. ADAD2 co‐localizes and forms novel granules with RNF17 in spermatocytes. Ablation of ADAD2 impairs the formation of RNF17 granules, decreases the number of cluster‐derived pachytene piRNAs, and increases expression of ping‐pong‐derived piRNAs.Discussion and conclusionIn collaboration with RNF17 and other RNA‐binding proteins in spermatocytes, ADAD2 directly or indirectly functions in piRNA biogenesis.

Funder

Takeda Science Foundation

Eunice Kennedy Shriver National Institute of Child Health and Human Development

Bill and Melinda Gates Foundation

Publisher

Wiley

Subject

Urology,Endocrinology,Reproductive Medicine,Endocrinology, Diabetes and Metabolism

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