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Published September 2, 2021 | Supplemental Material + Submitted + Published
Journal Article Open

RDC complex executes a dynamic piRNA program during Drosophila spermatogenesis to safeguard male fertility

Abstract

piRNAs are small non-coding RNAs that guide the silencing of transposons and other targets in animal gonads. In Drosophila female germline, many piRNA source loci dubbed "piRNA clusters" lack hallmarks of active genes and exploit an alternative path for transcription, which relies on the Rhino-Deadlock-Cutoff (RDC) complex. RDC was thought to be absent in testis, so it remains to date unknown how piRNA cluster transcription is regulated in the male germline. We found that components of RDC complex are expressed in male germ cells during early spermatogenesis, from germline stem cells (GSCs) to early spermatocytes. RDC is essential for expression of dual-strand piRNA clusters and transposon silencing in testis; however, it is dispensable for expression of Y-linked Suppressor of Stellate piRNAs and therefore Stellate silencing. Despite intact Stellate repression, males lacking RDC exhibited compromised fertility accompanied by germline DNA damage and GSC loss. Thus, piRNA-guided repression is essential for normal spermatogenesis beyond Stellate silencing. While RDC associates with multiple piRNA clusters in GSCs and early spermatogonia, its localization changes in later stages as RDC concentrates on a single X-linked locus, AT-chX. Dynamic RDC localization is paralleled by changes in piRNA cluster expression, indicating that RDC executes a fluid piRNA program during different stages of spermatogenesis. These results disprove the common belief that RDC is dispensable for piRNA biogenesis in testis and uncover the unexpected, sexually dimorphic and dynamic behavior of a core piRNA pathway machinery.

Additional Information

© 2021 Chen et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Received: November 1, 2020; Accepted: May 10, 2021; Published: September 2, 2021. We are grateful to Xin Chen, Peter Andersen, William Theurkauf, Trudi Schüpbach, Paul Lasko, Elena Pasyukova and three Drosophila Stock Centers (Bloomington, Vienna, Kyoto) for fly stocks. We thank Katalin Fejes Toth and members of Aravin lab for discussion and comments. We appreciate the help of Maria Ninova and Fan Gao (Bioinformatics Resource Center, Caltech) with bioinformatics analysis, the help of Grace Shin and Maayan Schwarzkopf with HCR experiments, the help of Giada Spigolon and Andres Collazo (Biological Imaging Facility, Caltech) with microscopy, and the help of Igor Antoshechkin (Millard and Muriel Jacobs Genetics and Genomics Laboratory, Caltech) with sequencing. Data Availability Statement: All data are available within the manuscript except for the sequencing data, which is available at NCBI SRA (accession number: PRJNA646006). This work was supported by the Howard Hughes Medical Institute Faculty Scholar Award (https://www.hhmi.org) and the National Institutes of Health R01 GM097363 (https://www.nih.gov) to AAA. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. Author Contributions: Conceptualization: Peiwei Chen, Alexei A. Aravin. Data curation: Peiwei Chen, Alexei A. Aravin. Formal analysis: Peiwei Chen, Alexei A. Aravin. Funding acquisition: Alexei A. Aravin. Investigation: Peiwei Chen, Yicheng Luo. Methodology: Peiwei Chen, Alexei A. Aravin. Project administration: Peiwei Chen, Alexei A. Aravin. Resources: Peiwei Chen, Alexei A. Aravin. Software: Peiwei Chen, Alexei A. Aravin. Supervision: Peiwei Chen, Alexei A. Aravin. Validation: Peiwei Chen, Yicheng Luo, Alexei A. Aravin. Visualization: Peiwei Chen, Alexei A. Aravin. Writing – original draft: Peiwei Chen, Alexei A. Aravin. Writing – review & editing: Peiwei Chen, Alexei A. Aravin. The authors have declared that no competing interests exist.

Attached Files

Published - journal.pgen.1009591.pdf

Submitted - 2020.08.25.266643v1.full.pdf

Supplemental Material - journal.pgen.1009591.s001.tif

Supplemental Material - journal.pgen.1009591.s002.tif

Supplemental Material - journal.pgen.1009591.s003.tif

Supplemental Material - journal.pgen.1009591.s004.tif

Supplemental Material - journal.pgen.1009591.s005.tif

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Additional details

Created:
August 20, 2023
Modified:
December 22, 2023