Sumoylation and its regulation in testicular Sertoli cells

相扑蛋白 支持细胞 细胞生物学 生物 细胞凋亡 调节器 泛素 精子发生 遗传学 基因 内分泌学
作者
Amitabha Sengupta,Manveet Nanda,Shanza Baseer Tariq,Tania Kiesel,Kayla Perlmutter,Margarita Vigodner
出处
期刊:Biochemical and Biophysical Research Communications [Elsevier]
卷期号:580: 56-62 被引量:3
标识
DOI:10.1016/j.bbrc.2021.09.066
摘要

The molecular regulation of Sertoli cells and their crosstalk with germ cells has not been fully characterized. SUMO proteins are essential for normal development and are expressed in mouse and human Sertoli cells; However, the cell-specific role of sumoylation in those cells has only started to be elucidated. In other cell types, including granulosa cells, sumoylation is regulated by a SUMO ligase KAP1/Trim28. Deletion of KAP1 in Sertoli cells causes testicular degeneration; However, the role of KAP1 in those cells has not been identified. Here we show that both mouse and human Sertoli undergo apoptosis upon inhibition of sumoylation with a chemical inhibitor or via a siRNA technology. We have additionally detected changes in the Sertoli cell proteome upon the inhibition of sumoylation, and our data suggest that among others, the expression of ER/stress-related proteins is highly affected by this inhibition. Sumoylation may also regulate the NOTCH signaling which is important for the maintenance of the developing germ cells. Furthermore, we show that a siRNA-down-regulation of KAP1 in a Sertoli-derived cell line causes an almost complete inactivation of sumoylation. In conclusion, sumoylation regulates important survival and signaling pathways in Sertoli cells, and KAP1 can be a major regulator of sumoylation in these cells.
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