Characterization of the Coronavirus Mouse Hepatitis Virus Strain A59 Small Membrane Protein E

doi:10.1128/JVI.74.5.2333-2342.2000

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Journal of Virology, March 2000, p. 2333-2342, Vol. 74, No. 5
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Characterization of the Coronavirus Mouse Hepatitis Virus Strain A59 Small Membrane Protein E

Martin J. B. Raamsman,¹ Jacomine Krijnse Locker,² Alphons de Hooge,¹ Antoine A. F. de Vries,¹ Gareth Griffiths,² Harry Vennema,¹ and Peter J. M. Rottier¹^,^*

Department of Infectious Diseases and Immunology, Faculty of Veterinary Medicine, Institute of Virology, and Institute of Biomembranes, Utrecht University, 3584 CL Utrecht, The Netherlands,¹ and European Molecular Biology Laboratory, Heidelberg, Germany²

Received 23 June 1999/Accepted 2 December 1999

The small envelope (E) protein has recently been shown to play an essential role in the assembly of coronaviruses. Expressionstudies revealed that for formation of the viral envelope, actuallyonly the E protein and the membrane (M) protein are required.Since little is known about this generally low-abundance virioncomponent, we have characterized the E protein of mouse hepatitisvirus strain A59 (MHV-A59), an 83-residue polypeptide. Using anantiserum to the hydrophilic carboxy terminus of this otherwisehydrophobic protein, we found that the E protein was synthesizedin infected cells with similar kinetics as the other viral structuralproteins. The protein appeared to be quite stable both duringinfection and when expressed individually using a vaccinia virusexpression system. Consistent with the lack of a predicted cleavagesite, the protein was found to become integrated in membraneswithout involvement of a cleaved signal peptide, nor were anyother modifications of the polypeptide observed. Immunofluorescenceanalysis of cells expressing the E protein demonstrated that thehydrophilic tail is exposed on the cytoplasmic side. Accordingly,this domain of the protein could not be detected on the outsideof virions but appeared to be inside, where it was protected fromproteolytic degradation. The results lead to a topological modelin which the polypeptide is buried within the membrane, spanningthe lipid bilayer once, possibly twice, and exposing only itscarboxy-terminal domain. Finally, electron microscopic studiesdemonstrated that expression of the E protein in cells inducedthe formation of characteristic membrane structures also observedin MHV-A59-infected cells, apparently consisting of masses oftubular, smooth, convoluted membranes. As judged by their colabelingwith antibodies to E and to Rab-1, a marker for the intermediatecompartment and endoplasmic reticulum, the E protein accumulatesin and induces curvature into these pre-Golgi membranes wherecoronaviruses have been shown earlier to assemble bybudding.

^* Corresponding author. Mailing address: Institute of Virology, Faculty of Veterinary Medicine, Utrecht University, P.O. Box80.165, 3508 TD Utrecht, The Netherlands. Phone: 31-30-2532462.Fax: 31-30-2536723. E-mail: P.Rottier{at}vet.uu.nl.

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