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piRNAs are crucial for transposon silencing, germ cell maturation, and fertility in male mice. Here, we report on the genetic landscape of piRNA dysfunction in humans and present 39 infertile men carrying biallelic variants in 14 different piRNA pathway genes, including PIWIL1, GTSF1, GPAT2, MAEL, TDRD1, and DDX4. In some affected men, the testicular phenotypes differ from those of the respective knockout mice and range from complete germ cell loss to the production of a few morphologically abnormal sperm. A reduced number of pachytene piRNAs was detected in the testicular tissue of variant carriers, demonstrating impaired piRNA biogenesis. Furthermore, LINE1 expression in spermatogonia links impaired piRNA biogenesis to transposon de-silencing and serves to classify variants as functionally relevant. These results establish the disrupted piRNA pathway as a major cause of human spermatogenic failure and provide insights into transposon silencing in human male germ cells.
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Birgit Stallmeyer
Institute of Human Genetics
Clara Bühlmann
University of Münster
Rytis Stakaitis
Lithuanian University of Health Sciences
Nature Communications
Inserm
University of Edinburgh
Radboud University Nijmegen
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Stallmeyer et al. (Fri,) studied this question.
synapsesocial.com/papers/68e5cda6b6db643587563573 — DOI: https://doi.org/10.1038/s41467-024-50930-9