Literature DB >> 28402725

Visualization of PML nuclear import complexes reveals FG-repeat nucleoporins at cargo retrieval sites.

Anna Lång1,2, Jens Eriksson1, Kay Oliver Schink3, Emma Lång1, Pernille Blicher1, Anna Połeć1, Andreas Brech3, Bjørn Dalhus1, Stig Ove Bøe1.   

Abstract

Selective nuclear import in eukaryotic cells involves sequential interactions between nuclear import receptors and phenylalanine-glycine (FG)-repeat nucleoporins. Traditionally, binding of cargoes to import receptors is perceived as a nuclear pore complex independent event, while interactions between import complexes and nucleoporins are thought to take place at the nuclear pores. However, studies have shown that nucleoporins are mobile and not static within the nuclear pores, suggesting that they may become engaged in nuclear import before nuclear pore entry. Here we have studied post-mitotic nuclear import of the tumor suppressor protein PML. Since this protein forms nuclear compartments called PML bodies that persist during mitosis, the assembly of putative PML import complexes can be visualized on the surface of these protein aggregates as the cell progress from an import inactive state in mitosis to an import active state in G1. We show that these post-mitotic cytoplasmic PML bodies incorporate a multitude of peripheral nucleoporins, but not scaffold or nuclear basket nucleoporins, in a manner that depends on FG-repeats, the KPNB1 import receptor, and the PML nuclear localization signal. The study suggests that nucleoporins have the ability to target certain nuclear cargo proteins in a nuclear pore-uncoupled state, before nuclear pore entry.

Entities:  

Keywords:  FG-repeats; KPNB1; PML; PML bodies; nuclear import; nuclear pore complex; nucleoporins

Mesh:

Substances:

Year:  2017        PMID: 28402725      PMCID: PMC5597291          DOI: 10.1080/19491034.2017.1306161

Source DB:  PubMed          Journal:  Nucleus        ISSN: 1949-1034            Impact factor:   4.197


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