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Annulate lamellae play only a minor role in the storage of excess nucleoporins in Drosophila embryos
Södertörn University, School of Chemistry, Biology, Geography and Environmental Science. Karolinska Institute.
Institute of Cytology and Genetics, Novosibirsk, Russia.
Karolinska Institute.
Institute of Cytology and Genetics, Novosibirsk, Russia.
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2004 (English)In: Traffic: the International Journal of Intracellular Transport, ISSN 1398-9219, E-ISSN 1600-0854, Vol. 5, no 3, p. 152-164Article in journal (Refereed) Published
Abstract [en]

The nuclear pore complexes (NPCs), multiprotein assemblies embedded in the nuclear envelope, conduct nucleo-cytoplasmic traffic of macromolecules. Mimics of NPCs, called annulate lamellae pore complexes (ALPCs), are usually found in cytoplasmic membranous stacks in oocytes and early embryonic cells. They are believed to constitute storage compartments for excess premade nucleoporins. To evaluate the extent to which ALPCs store nucleoporins in early embryonic cells we took advantage of syncytial Drosophila embryos, containing both AL and rapidly proliferating nuclei in the common cytoplasm. Electron microscopic morphometric analysis showed that the number of ALPCs did not decrease to compensate for the growing number of NPCs during syncytial development. We performed Western blot analysis to quantify seven different nucleoporins and analyzed their intraembryonal distribution by confocal microscopy and subcellular fractionation. Syncytial embryos contained a large maternally contributed stockpile of nucleoporins. However, even during interphases, only a small fraction of the excess nucleoporins was assembled into ALPCs, whereas the major fraction was soluble and contained at least one phosphorylated nucleoporin. We conclude that in Drosophila embryos ALPCs play only a minor role in storing the excess maternally contributed nucleoporins. Factors that may prevent nucleoporins from assembly into ALPCs are discussed.

Place, publisher, year, edition, pages
2004. Vol. 5, no 3, p. 152-164
National Category
Cell Biology
Identifiers
URN: urn:nbn:se:sh:diva-15486DOI: 10.1111/j.1600-0854.2004.0166.xISI: 000189142900004PubMedID: 15086791Scopus ID: 2-s2.0-1642376626OAI: oai:DiVA.org:sh-15486DiVA, id: diva2:504572
Available from: 2012-02-21 Created: 2012-02-20 Last updated: 2017-12-07Bibliographically approved
In thesis
1. Disassembly and reassembly of the nuclear pore complex
Open this publication in new window or tab >>Disassembly and reassembly of the nuclear pore complex
2006 (English)Doctoral thesis, comprehensive summary (Other academic)
Abstract [en]

The nuclear pore complexes (NPCs) are multiprotein communicative channels spanning the nuclear envelope. In higher eukaryotes NPCs reversibly disassemble during mitosis into distinct nucleoporin subcomplexes. Some cell types (e.g. oocytes and early embryonic cells) also contain mimics of NPCs of unknown function, which are located in cytoplasmic membranes. They are termed annulate lamellae pore complexes (ALPC). This study was aimed at understanding the process of mitotic disassembly and reassembly of the NPC and at elucidating the function of ALPCs. Using syncytial Drosophila embryos as a model we have tested the proposed function of ALPCs as a storage compartment for nucleoporins fueling assembly of new NPCs in rapidly proliferating cells. Surprisingly, we found that ALPCs are not depleted during assembly of new NPCs and that they represent only a minor fraction of the total embryonic nucleoporins while the major fraction is persistently soluble. We conclude that in Drosophila, ALPCs play only a minor role as a storage compartment for nucleoporins. We developed a novel in vivo model system based on syncytial Drosophila embryos to study mitotic disassembly/reassembly of the NPC. We found that the major mitotic kinase Cdk1 is the key regulator of both NPC and ALPC disassembly/reassembly in vivo and that Cdk1 activity is able to phosphorylate and solubilize nucleoporins in vitro. We also found that phosphatase activity, sensitive to okadaic acid (OA), is required for reassembly of both NPCs and ALPCs in vivo. Additionally, we showed that the Ran GTPase system, that drives active nucleocytoplasmic transport during intephase, is selectively required for post-mitotic reassembly of NPCs but not ALPCs in vivo. Our findings suggest that in live cells NPC assembly is regulated by a dynamic equilibrium between kinase (Cdk1) and phospahatase (sensitive to OA) activity and that it is spatially coordinated by the Ran GTPase system. Finally. using the nucleoporin gp210 as a model. we have tested a role of mitotic phosphorylation of nucleoporins in disassembly of the NPC. We present evidence that a single mitotic phosphorylation of gp210 weakens its binding to the NPC and interferes with its postmitotic recruitment to the newly formed NE. These findings represent the first direct evidence that mitotic nucleoporin phosphorylation functions in disassembly of the NPC.

Place, publisher, year, edition, pages
Stockholm: Karolinska instiutet, 2006. p. 65
National Category
Biological Sciences
Identifiers
urn:nbn:se:sh:diva-31961 (URN)91-7140-929-7 (ISBN)
Public defence
2006-10-13, MA648, Alfred Nobels allé 7, Huddinge, 09:00 (English)
Opponent
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Available from: 2017-02-06 Created: 2017-02-06 Last updated: 2017-02-06Bibliographically approved

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Onischenko, Evgeny AHallberg, Einar

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