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The SUMO-specific isopeptidase SENP2 is targeted to intracellular membranes via a predicted N-terminal amphipathic α-helix

机译:SUMO特异性异肽酶SENP2通过预测的N末端两亲性α-螺旋靶向细胞内膜

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摘要

Sumoylation regulates a wide range of essential cellular functions, many of which are associated with activities in the nucleus. Although there is also emerging evidence for the involvement of the small ubiquitin-related modifier (SUMO) at intracellular membranes, the mechanisms by which sumoylation is regulated at membranes is largely unexplored. In this study, we report that the SUMO-specific isopeptidase, SENP2, uniquely associates with intracellular membranes. Using in vivo analyses and in vitro binding assays, we show that SENP2 is targeted to intracellular membranes via a predicted N-terminal amphipathic α-helix that promotes direct membrane binding. Furthermore, we demonstrate that SENP2 binding to intracellular membranes is regulated by interactions with the nuclear import receptor karyopherin-α. Consistent with membrane association, biotin identification (BioID) revealed interactions between SENP2 and endoplasmic reticulum, Golgi, and inner nuclear membrane-associated proteins. Collectively, our findings indicate that SENP2 binds to intracellular membranes where it interacts with membrane-associated proteins and has the potential to regulate their sumoylation and membrane-associated functions.
机译:糖基化调节广泛的基本细胞功能,其中许多功能与细胞核中的活性有关。尽管也有新的证据表明小泛素相关修饰剂(SUMO)参与细胞内膜,但在膜上调节磺酰化的机制尚不清楚。在这项研究中,我们报告了SUMO特异性异肽酶SENP2与细胞内膜独特地相关。使用体内分析和体外结合测定,我们显示SENP2通过预测的N端两亲性α-螺旋促进细胞膜直接结合,靶向细胞内膜。此外,我们证明与细胞内膜结合的SENP2受与核输入受体核转运蛋白-α相互作用的调节。与膜结合一致,生物素识别(BioID)显示SENP2与内质网,高尔基体和内核膜相关蛋白之间存在相互作用。总的来说,我们的发现表明SENP2结合到细胞内膜上,在膜上它与膜相关蛋白相互作用,并有可能调节它们的磺酰化和膜相关功能。

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