[No authors listed]
Stimulated by retinoic acid 8 (Stra8), one of genes induced by retinoic acid (RA), is required for the meiotic initiation of male spermatogenesis. The present study found that Stra8 inhibited apoptosis in male Stra8âknockout mice, and in mice with vitamin A deficiency and vitamin A recovery in vivo. This phenotype was also verified in GC1 spermatogonia (spg) cells overexpressing Stra8. In addition, microarray analysis identified that there were nine differentially expressed genes (DEGs) in the Stra8âoverexpressed GC1 spg cells compared with the control groups; the expression of these nine genes was verified via mRNA expression levels. The DEGs were as follows: Phosphatidylinositolâdependent kinase 1 (PDK1), a key gene upstream of protein kinase B (AKT); angiopoietin 2, a Bâcell lymphoma 2 (Bclâ2)âinhibited gene; transcription factor 4, glutathione Sâtransferase P91 and ubiquitinâspecific protease 33, mitogenâactivated protein kinase (MAPK)ârelated genes; oxidative stress induced growth inhibitor 1, related to the P53 pathway; Bclâ2, P53, ERK (MAPK1/3), câJun Nâterminal kinase (MAPK8/9), and P38 (MAPK14), all of which are key genes involved in the AKT signaling pathway. Therefore, the present study further verified these genes and found that the mRNA and protein expression levels of PDK1, AKT, Bclâ2 and ERK were increased. Although the mRNA expression level of P53 was decreased, there was no significant difference in the protein expression level in Stra8âoverexpressing GC1 spg cells compared with controls. In addition, Caspase 3, one of the executioner caspases, was decreased in Stra8âoverexpressing GC1 spg cells compared with the control groups. Therefore, it was suggested that Stra8 may directly or indirectly inhibit caspases through the AKT signaling pathway and ultimately exert an antiâapoptotic effect in the male reproductive system.
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