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* To whom correspondence should be addressed. E-mail: khkim{at}wsu.edu.
Covalent attachment of small ubiquitin-related modifier (SUMO) to target proteins is an important post-translational mechanism controlling diverse cellular functions. Recently, hypo- or hyper-sumoylation by SUMO-2/3 was shown to play a crucial role in male reproduction. However, the regulation of SUMO-2/3 in the testis remains unknown. Here, we report that the subcellular localization of SUMO-2/3 changes during testicular development. SUMO-2/3 was mainly found localized in the nucleus of Sertoli cells and gonocytes, early in testicular development, but the localization shifted to the cytoplasm in Sertoli and germ cells after meiotic initiation. This change in the subcellular localization was mimicked both in testes of postnatal-day-10 (P10) rats, injected with all-trans retinoic acid (ATRA), and in organ cultures of testes from P10 rats treated with ATRA. These results suggest that retinoic acid may have a role in controlling the subcellular localization of SUMO-2/3. Moreover, treatment of Sertoli cells with a RARA-specific agonist changed the subcellular localization of SUMO-2/3 from the nucleus to the cytoplasm. Furthermore, disruption of retinoic acid receptor alpha (Rara) gene in the testis resulted in alteration of SUMO-2/3 subcellular localization, indicating that its protein RARA may have a role in the nuclear trafficking of SUMO-2/3. Since many SUMO target proteins are usually modified en masse after a biological stimulus, our results suggest that dysregulation of SUMO-2/3 subcellular localization could easily be a pleiotropic contributing factor that can cause a male sterility phenotype in Rara-null mice.
Key words: Infertility •
Spermatogenesis •
Testis
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