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Literature DB >> 12941687

Gangliosides are receptors for murine polyoma virus and SV40.

Billy Tsai¹, Joanna M Gilbert, Thilo Stehle, Wayne Lencer, Thomas L Benjamin, Tom A Rapoport.

Abstract

Polyoma virus (Py) and simian virus 40 (SV40) travel from the plasma membrane to the endoplasmic reticulum (ER) from where they enter the cytosol and then the nucleus to initiate infection. Here we demonstrate that specific gangliosides can serve as plasma membrane receptors for these viruses, GD1a and GT1b for Py and GM1 for SV40. Binding and flotation assays were used to show that addition of these gangliosides to phospholipid vesicles allowed specific binding of the respective viruses. The crystal structure of polyoma VP1 with a sialic acid-containing oligosaccharide was used to derive a model of how the two terminal sugars (sialic acid-alpha2,3-galactose) in one branch of GD1a and GT1b are recognized by the virus. A rat cell line deficient in ganglioside synthesis is poorly infectible by polyoma and SV40, but addition of the appropriate gangliosides greatly facilitates virus uptake, transport to the ER and infection. Lipid binding sites for polyoma are shown to be present in rough ER membranes, suggesting that the virus travel with the ganglioside(s) from the plasma membranes to the ER.

Entities: Chemical Disease Species

Mesh：

Substances：

Year: 2003 PMID： 12941687 PMCID： PMC202381 DOI： 10.1093/emboj/cdg439

Source DB: PubMed Journal: EMBO J ISSN： 0261-4189 Impact factor: 11.598

40 in total

1. Protein disulfide isomerase acts as a redox-dependent chaperone to unfold cholera toxin.

Authors: B Tsai; C Rodighiero; W I Lencer; T A Rapoport
Journal: Cell Date: 2001-03-23 Impact factor: 41.582

Review 2. Combinatorial ganglioside biosynthesis.

Authors: Thomas Kolter; Richard L Proia; Konrad Sandhoff
Journal: J Biol Chem Date: 2002-05-13 Impact factor: 5.157

Review 3. Common principles in viral entry.

Authors: Minna M Poranen; Rimantas Daugelavicius; Dennis H Bamford
Journal: Annu Rev Microbiol Date: 2002-01-30 Impact factor: 15.500

4. Inhibitors of COP-mediated transport and cholera toxin action inhibit simian virus 40 infection.

Authors: Ayanthi A Richards; Espen Stang; Rainer Pepperkok; Robert G Parton
Journal: Mol Biol Cell Date: 2002-05 Impact factor: 4.138

5. Early steps of polyomavirus entry into cells.

Authors: J M Gilbert; T L Benjamin
Journal: J Virol Date: 2000-09 Impact factor: 5.103

6. Uncoupling of the cholera toxin-G(M1) ganglioside receptor complex from endocytosis, retrograde Golgi trafficking, and downstream signal transduction by depletion of membrane cholesterol.

Authors: Anne A Wolf; Yukako Fujinaga; Wayne I Lencer
Journal: J Biol Chem Date: 2002-02-21 Impact factor: 5.157

7. Caveolar endocytosis of simian virus 40 reveals a new two-step vesicular-transport pathway to the ER.

Authors: L Pelkmans; J Kartenbeck; A Helenius
Journal: Nat Cell Biol Date: 2001-05 Impact factor: 28.824

8. Caveolar endocytosis of simian virus 40 is followed by brefeldin A-sensitive transport to the endoplasmic reticulum, where the virus disassembles.

Authors: Leonard C Norkin; Howard A Anderson; Scott A Wolfrom; Ariella Oppenheim
Journal: J Virol Date: 2002-05 Impact factor: 5.103

9. Mouse polyomavirus utilizes recycling endosomes for a traffic pathway independent of COPI vesicle transport.

Authors: Petra Mannová; Jitka Forstová
Journal: J Virol Date: 2003-02 Impact factor: 5.103

10. Unfolded cholera toxin is transferred to the ER membrane and released from protein disulfide isomerase upon oxidation by Ero1.

Authors: Billy Tsai; Tom A Rapoport
Journal: J Cell Biol Date: 2002-10-28 Impact factor: 10.539

175 in total

Review 1. Endoplasmic reticulum-dependent redox reactions control endoplasmic reticulum-associated degradation and pathogen entry.

Authors: Christopher P Walczak; Kaleena M Bernardi; Billy Tsai
Journal: Antioxid Redox Signal Date: 2012-01-30 Impact factor: 8.401

2. Retrograde transport of cholera toxin from the plasma membrane to the endoplasmic reticulum requires the trans-Golgi network but not the Golgi apparatus in Exo2-treated cells.

Authors: Yan Feng; Ashutosh P Jadhav; Chiara Rodighiero; Yukako Fujinaga; Tomas Kirchhausen; Wayne I Lencer
Journal: EMBO Rep Date: 2004-05-21 Impact factor: 8.807

Gangliosides are receptors for murine polyoma virus and SV40.

1. Protein disulfide isomerase acts as a redox-dependent chaperone to unfold cholera toxin.

Review 2. Combinatorial ganglioside biosynthesis.

Review 3. Common principles in viral entry.

4. Inhibitors of COP-mediated transport and cholera toxin action inhibit simian virus 40 infection.

5. Early steps of polyomavirus entry into cells.

6. Uncoupling of the cholera toxin-G(M1) ganglioside receptor complex from endocytosis, retrograde Golgi trafficking, and downstream signal transduction by depletion of membrane cholesterol.

7. Caveolar endocytosis of simian virus 40 reveals a new two-step vesicular-transport pathway to the ER.

8. Caveolar endocytosis of simian virus 40 is followed by brefeldin A-sensitive transport to the endoplasmic reticulum, where the virus disassembles.

9. Mouse polyomavirus utilizes recycling endosomes for a traffic pathway independent of COPI vesicle transport.

10. Unfolded cholera toxin is transferred to the ER membrane and released from protein disulfide isomerase upon oxidation by Ero1.

Review 1. Endoplasmic reticulum-dependent redox reactions control endoplasmic reticulum-associated degradation and pathogen entry.

2. Retrograde transport of cholera toxin from the plasma membrane to the endoplasmic reticulum requires the trans-Golgi network but not the Golgi apparatus in Exo2-treated cells.

3. Cholera toxin toxicity does not require functional Arf6- and dynamin-dependent endocytic pathways.

4. BAP31 and BiP are essential for dislocation of SV40 from the endoplasmic reticulum to the cytosol.

5. A PDI family network acts distinctly and coordinately with ERp29 to facilitate polyomavirus infection.

6. Dimerization of ERp29, a PDI-like protein, is essential for its diverse functions.

7. Simian virus 40 infection triggers a balanced network that includes apoptotic, survival, and stress pathways.

8. Gangliosides and beta1-integrin are required for caveolae and membrane domains.

Review 9. Rules and exceptions: sialic acid variants and their role in determining viral tropism.

10. Gangliosides as high affinity receptors for tetanus neurotoxin.