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Literature DB >> 16000379

Interaction between the shuttling mRNA export factor Gle1 and the nucleoporin hCG1: a conserved mechanism in the export of Hsp70 mRNA.

Frederic Kendirgi¹, Deborah J Rexer, Abel R Alcázar-Román, Halina M Onishko, Susan R Wente.

Abstract

Translocation of messenger RNAs through the nuclear pore complex (NPC) requires coordinated physical interactions between stable NPC components, shuttling transport factors, and mRNA-binding proteins. In budding yeast (y) and human (h) cells, Gle1 is an essential mRNA export factor. Nucleocytoplasmic shuttling of hGle1 is required for mRNA export; however, the mechanism by which hGle1 associates with the NPC is unknown. We have previously shown that the interaction of hGle1 with the nucleoporin hNup155 is necessary but not sufficient for targeting hGle1 to NPCs. Here, we report that the unique C-terminal 43 amino acid region of the hGle1B isoform mediates binding to the C-terminal non-FG region of the nucleoporin hCG1/NPL1. Moreover, hNup155, hGle1B, and hCG1 formed a heterotrimeric complex in vitro. This suggested that these two nucleoporins were required for the NPC localization of hGle1. Using an siRNA-based approach, decreased levels of hCG1 resulted in hGle1 accumulation in cytoplasmic foci. This was coincident with inhibition of heat shock-induced production of Hsp70 protein and export of the Hsp70 mRNA in HeLa cells. Because this closely parallels the role of the hCG1 orthologue yNup42/Rip1, we speculate that hGle1-hCG1 function in the mRNA export mechanism is highly conserved.

Entities: Gene Species

Mesh：

Substances：

Year: 2005 PMID： 16000379 PMCID： PMC1196339 DOI： 10.1091/mbc.e04-11-0998

Source DB: PubMed Journal: Mol Biol Cell ISSN： 1059-1524 Impact factor: 4.138

72 in total

1. Nup116p and nup100p are interchangeable through a conserved motif which constitutes a docking site for the mRNA transport factor gle2p.

Authors: S M Bailer; S Siniossoglou; A Podtelejnikov; A Hellwig; M Mann; E Hurt
Journal: EMBO J Date: 1998-02-16 Impact factor: 11.598

2. Dbp5p/Rat8p is a yeast nuclear pore-associated DEAD-box protein essential for RNA export.

Authors: C A Snay-Hodge; H V Colot; A L Goldstein; C N Cole
Journal: EMBO J Date: 1998-05-01 Impact factor: 11.598

3. Mex67p, a novel factor for nuclear mRNA export, binds to both poly(A)+ RNA and nuclear pores.

Authors: A Segref; K Sharma; V Doye; A Hellwig; J Huber; R Lührmann; E Hurt
Journal: EMBO J Date: 1997-06-02 Impact factor: 11.598

4. Yeast heat shock mRNAs are exported through a distinct pathway defined by Rip1p.

Authors: C A Saavedra; C M Hammell; C V Heath; C N Cole
Journal: Genes Dev Date: 1997-11-01 Impact factor: 11.361

5. The yeast nucleoporin rip1p contributes to multiple export pathways with no essential role for its FG-repeat region.

Authors: F Stutz; J Kantor; D Zhang; T McCarthy; M Neville; M Rosbash
Journal: Genes Dev Date: 1997-11-01 Impact factor: 11.361

6. Rat8p/Dbp5p is a shuttling transport factor that interacts with Rat7p/Nup159p and Gle1p and suppresses the mRNA export defect of xpo1-1 cells.

Authors: C A Hodge; H V Colot; P Stafford; C N Cole
Journal: EMBO J Date: 1999-10-15 Impact factor: 11.598

7. Genomic libraries and a host strain designed for highly efficient two-hybrid selection in yeast.

Authors: P James; J Halladay; E A Craig
Journal: Genetics Date: 1996-12 Impact factor: 4.562

8. GLE2, a Saccharomyces cerevisiae homologue of the Schizosaccharomyces pombe export factor RAE1, is required for nuclear pore complex structure and function.

Authors: R Murphy; J L Watkins; S R Wente
Journal: Mol Biol Cell Date: 1996-12 Impact factor: 4.138

9. Cytoplasmic inositol hexakisphosphate production is sufficient for mediating the Gle1-mRNA export pathway.

Authors: Aimee L Miller; Mythili Suntharalingam; Sylvia L Johnson; Anjon Audhya; Scott D Emr; Susan R Wente
Journal: J Biol Chem Date: 2004-09-30 Impact factor: 5.157

10. The human homologue of Saccharomyces cerevisiae Gle1p is required for poly(A)+ RNA export.

Authors: J L Watkins; R Murphy; J L Emtage; S R Wente
Journal: Proc Natl Acad Sci U S A Date: 1998-06-09 Impact factor: 11.205

47 in total

1. Following temperature stress, export of heat shock mRNA occurs efficiently in cells with mutations in genes normally important for mRNA export.

Authors: Christiane Rollenhagen; Christine A Hodge; Charles N Cole
Journal: Eukaryot Cell Date: 2007-01-26

Review 2. mRNA nuclear export at a glance.

Authors: Sean R Carmody; Susan R Wente
Journal: J Cell Sci Date: 2009-06-15 Impact factor: 5.285

Interaction between the shuttling mRNA export factor Gle1 and the nucleoporin hCG1: a conserved mechanism in the export of Hsp70 mRNA.

1. Nup116p and nup100p are interchangeable through a conserved motif which constitutes a docking site for the mRNA transport factor gle2p.

2. Dbp5p/Rat8p is a yeast nuclear pore-associated DEAD-box protein essential for RNA export.

3. Mex67p, a novel factor for nuclear mRNA export, binds to both poly(A)+ RNA and nuclear pores.

4. Yeast heat shock mRNAs are exported through a distinct pathway defined by Rip1p.

5. The yeast nucleoporin rip1p contributes to multiple export pathways with no essential role for its FG-repeat region.

6. Rat8p/Dbp5p is a shuttling transport factor that interacts with Rat7p/Nup159p and Gle1p and suppresses the mRNA export defect of xpo1-1 cells.

7. Genomic libraries and a host strain designed for highly efficient two-hybrid selection in yeast.

8. GLE2, a Saccharomyces cerevisiae homologue of the Schizosaccharomyces pombe export factor RAE1, is required for nuclear pore complex structure and function.

9. Cytoplasmic inositol hexakisphosphate production is sufficient for mediating the Gle1-mRNA export pathway.

10. The human homologue of Saccharomyces cerevisiae Gle1p is required for poly(A)+ RNA export.

1. Following temperature stress, export of heat shock mRNA occurs efficiently in cells with mutations in genes normally important for mRNA export.

Review 2. mRNA nuclear export at a glance.

3. mRNA nuclear export and human disease.

Review 4. The Structure of the Nuclear Pore Complex (An Update).

5. Nup42 and IP₆ coordinate Gle1 stimulation of Dbp5/DDX19B for mRNA export in yeast and human cells.

Review 6. Postage for the messenger: designating routes for nuclear mRNA export.

7. Nucleoporin FG domains facilitate mRNP remodeling at the cytoplasmic face of the nuclear pore complex.

8. Mutations in mRNA export mediator GLE1 result in a fetal motoneuron disease.

9. The oncogene eIF4E reprograms the nuclear pore complex to promote mRNA export and oncogenic transformation.

10. Nuclear export factor RBM15 facilitates the access of DBP5 to mRNA.