Literature DB >> 9371630

Oligomerization-dependent folding of the membrane fusion protein of Semliki Forest virus.

H Andersson1, B U Barth, M Ekström, H Garoff.   

Abstract

The spikes of alphaviruses are composed of three copies of an E2-E1 heterodimer. The E1 protein possesses membrane fusion activity, and the E2 protein, or its precursor form, p62 (sometimes called PE2), controls this function. Both proteins are, together with the viral capsid protein, translated from a common C-p62-E1 coding unit. In an earlier study, we showed that the p62 protein of Semliki Forest virus (SFV) dimerizes rapidly and efficiently in the endoplasmic reticulum (ER) with the E1 protein originating from the same translation product (so-called heterodimerization in cis) (B.-U. Barth, J. M. Wahlberg, and H. Garoff, J. Cell Biol. 128:283-291, 1995). In the present work, we analyzed the ER translocation and folding efficiencies of the p62 and E1 proteins of SFV expressed from separate coding units versus a common one. We found that the separately expressed p62 protein translocated and folded almost as efficiently as when it was expressed from a common coding unit, whereas the independently expressed E1 protein was inefficient in both processes. In particular, we found that the majority of the translocated E1 chains were engaged in disulfide-linked aggregates. This result suggests that the E1 protein needs to form a complex with p62 to avoid aggregation. Further analyses of the E1 aggregation showed that it occurred very rapidly after E1 synthesis and could not be avoided significantly by the coexpression of an excess of p62 from a separate coding unit. These latter results suggest that the p62-E1 heterodimerization has to occur very soon after E1 synthesis and that this is possible only in a cis-directed reaction which follows the synthesis of p62 and E1 from a common coding unit. We propose that the p62 protein, whose synthesis precedes that of the E1 protein, remains in the translocon of the ER and awaits the completion of E1. This strategy enables the p62 protein to complex with the E1 protein immediately after the latter has been made and thereby to control (suppress) its fusion activity.

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Year:  1997        PMID: 9371630      PMCID: PMC230274     

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  77 in total

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Authors:  S L Allison; J Schalich; K Stiasny; C W Mandl; C Kunz; F X Heinz
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3.  Semliki Forest virus particles containing only the E1 envelope glycoprotein are infectious and can induce cell-cell fusion.

Authors:  A Omar; H Koblet
Journal:  Virology       Date:  1988-09       Impact factor: 3.616

4.  The cotranslational integration of membrane proteins into the phospholipid bilayer is a multistep process.

Authors:  H Do; D Falcone; J Lin; D W Andrews; A E Johnson
Journal:  Cell       Date:  1996-05-03       Impact factor: 41.582

5.  Identification of distinct antigenic determinants on Semliki Forest virus by using monoclonal antibodies with different antiviral activities.

Authors:  W A Boere; T Harmsen; J Vinjé; B J Benaissa-Trouw; C A Kraaijeveld; H Snippe
Journal:  J Virol       Date:  1984-11       Impact factor: 5.103

6.  Reinitiation of translocation in the Semliki Forest virus structural polyprotein: identification of the signal for the E1 glycoprotein.

Authors:  P Melancon; H Garoff
Journal:  EMBO J       Date:  1986-07       Impact factor: 11.598

7.  Folding and oligomerization of influenza hemagglutinin in the ER and the intermediate compartment.

Authors:  U Tatu; C Hammond; A Helenius
Journal:  EMBO J       Date:  1995-04-03       Impact factor: 11.598

8.  Membrane fusion process of Semliki Forest virus. I: Low pH-induced rearrangement in spike protein quaternary structure precedes virus penetration into cells.

Authors:  J M Wahlberg; H Garoff
Journal:  J Cell Biol       Date:  1992-01       Impact factor: 10.539

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Authors:  I Braakman; H Hoover-Litty; K R Wagner; A Helenius
Journal:  J Cell Biol       Date:  1991-08       Impact factor: 10.539

10.  Posttranslational oligomerization and cooperative acid activation of mixed influenza hemagglutinin trimers.

Authors:  F Boulay; R W Doms; R G Webster; A Helenius
Journal:  J Cell Biol       Date:  1988-03       Impact factor: 10.539
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Authors:  Ivo C Lorenz; Steven L Allison; Franz X Heinz; Ari Helenius
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2.  Formation and characterization of the trimeric form of the fusion protein of Semliki Forest Virus.

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3.  The dynamic envelope of a fusion class II virus. E3 domain of glycoprotein E2 precursor in Semliki Forest virus provides a unique contact with the fusion protein E1.

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4.  Furin processing and proteolytic activation of Semliki Forest virus.

Authors:  Xinyong Zhang; Martin Fugère; Robert Day; Margaret Kielian
Journal:  J Virol       Date:  2003-03       Impact factor: 5.103

5.  MAR1 links membrane adhesion to membrane merger during cell-cell fusion in Chlamydomonas.

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6.  Structural plasticity of the Semliki Forest virus glycome upon interspecies transmission.

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7.  The disulfide bonds in glycoprotein E2 of hepatitis C virus reveal the tertiary organization of the molecule.

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8.  Role of conserved cysteines in the alphavirus E3 protein.

Authors:  Megan M Parrott; Sarah A Sitarski; Randy J Arnold; Lora K Picton; R Blake Hill; Suchetana Mukhopadhyay
Journal:  J Virol       Date:  2008-12-24       Impact factor: 5.103

9.  Lectin-mediated retention of p62 facilitates p62-E1 heterodimerization in endoplasmic reticulum of Semliki Forest virus-infected cells.

Authors:  Helena Andersson; Henrik Garoff
Journal:  J Virol       Date:  2003-06       Impact factor: 5.103

10.  4.4 Å cryo-EM structure of an enveloped alphavirus Venezuelan equine encephalitis virus.

Authors:  Rui Zhang; Corey F Hryc; Yao Cong; Xiangan Liu; Joanita Jakana; Rodion Gorchakov; Matthew L Baker; Scott C Weaver; Wah Chiu
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