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arrestin3 蛋白在细胞核内的泛素化触发了 Mdm2 的核输出,而 Mdm2 又反过来介导了细胞质中 GRK2 的泛素化。

The Ubiquitination of Arrestin3 within the Nucleus Triggers the Nuclear Export of Mdm2, Which, in Turn, Mediates the Ubiquitination of GRK2 in the Cytosol.

机构信息

Department of Pharmacology, College of Pharmacy, Chonnam National University, Gwang-Ju 61186, Republic of Korea.

出版信息

Int J Mol Sci. 2024 Sep 6;25(17):9644. doi: 10.3390/ijms25179644.

Abstract

GRK2 and arrestin3, key players in the functional regulation of G protein-coupled receptors (GPCRs), are ubiquitinated by Mdm2, a nuclear protein. The agonist-induced increase in arrestin3 ubiquitination occurs in the nucleus, underscoring the crucial role of its nuclear translocation in this process. The ubiquitination of arrestin3 occurs in the nucleus, highlighting the pivotal role of its nuclear translocation in this process. In contrast, GRK2 cannot translocate into the nucleus; thus, facilitation of the cytosolic translocation of nuclear Mdm2 is required to ubiquitinate GRK2 in the cytosol. Among the explored cellular components and processes, arrestin, Gβγ, clathrin, and receptor phosphorylation were found to be required for the nuclear import of arrestin3, the ubiquitination of arrestin3 in the nucleus, nuclear export of Mdm2, and the ubiquitination of GRK2 in the cytosol. In conclusion, our findings demonstrate that agonist-induced ubiquitination of arrestin3 in the nucleus is interconnected with cytosolic GRK2 ubiquitination.

摘要

GRK2 和 arrestin3 是 G 蛋白偶联受体 (GPCR) 功能调节的关键因子,它们被核蛋白 Mdm2 泛素化。激动剂诱导的 arrestin3 泛素化增加发生在细胞核中,突出了其核易位在这一过程中的关键作用。arrestin3 的泛素化发生在细胞核中,突出了其核易位在这一过程中的关键作用。相比之下,GRK2 不能易位到细胞核中;因此,需要促进核 Mdm2 的细胞质易位,以在细胞质中泛素化 GRK2。在探索的细胞成分和过程中,发现 arrestin、Gβγ、网格蛋白和受体磷酸化对于 arrestin3 的核内易位、细胞核内 arrestin3 的泛素化、Mdm2 的核输出以及细胞质中 GRK2 的泛素化是必需的。总之,我们的发现表明,激动剂诱导的细胞核内 arrestin3 泛素化与细胞质中 GRK2 泛素化相互关联。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9e16/11395016/4372638053f7/ijms-25-09644-g001.jpg

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