Spermatogonial Deubiquitinase USP9X is Essential for Proper Spermatogenesis in Mice

Overview

Journal Reproduction

Specialty Reproductive Medicine

Date 2017 Jun 1

PMID 28559472

Citations 18

Authors

Kasane Kishi

Aya Uchida

Hinako M Takase

Hitomi Suzuki

Masamichi Kurohmaru

Naoki Tsunekawa

Masami Kanai-Azuma

Stephen A Wood

Yoshiakira Kanai

Affiliations

Soon will be listed here.

Abstract

USP9X (ubiquitin-specific peptidase 9, X chromosome) is the mammalian orthologue of deubiquitinase fat facets that was previously shown to regulate the maintenance of the germ cell lineage partially through stabilizing Vasa, one of the widely conserved factors crucial for gametogenesis. Here, we demonstrate that USP9X is expressed in the gonocytes and spermatogonia in mouse testes from newborn to adult stages. By using mice, germ cell-specific conditional deletion of from the embryonic stage showed no abnormality in the developing testes by 1 week and no appreciable defects in the undifferentiated and differentiating spermatogonia at postnatal and adult stages. Interestingly, after 2 weeks, -null spermatogenic cells underwent apoptotic cell death at the early spermatocyte stage, and then, caused subsequent aberrant spermiogenesis, which resulted in a complete infertility of conditional knockout male mice. These data provide the first evidence of the crucial role of the spermatogonial USP9X during transition from the mitotic to meiotic phases and/or maintenance of early meiotic phase in conditional knockout testes.

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