Variations in Disparate Regions of the Murine Coronavirus Spike Protein Impact the Initiation of Membrane Fusion

doi:10.1128/JVI.75.6.2792-2802.2001

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Journal of Virology, March 2001, p. 2792-2802, Vol. 75, No. 6
0022-538X/01/$04.00+0 DOI: 10.1128/JVI.75.6.2792-2802.2001
Copyright © 2001, American Society for Microbiology. All rights reserved.

Variations in Disparate Regions of the Murine Coronavirus Spike Protein Impact the Initiation of Membrane Fusion

Dawn K. Krueger, Sean M. Kelly, Daniel N. Lewicki, Rosanna Ruffolo, and Thomas M. Gallagher^*

Department of Microbiology and Immunology, Loyola University Medical Center, Maywood, Illinois 60153

Received 7 July 2000/Accepted 18 December 2000

The prototype JHM strain of murine hepatitis virus (MHV) is an enveloped, RNA-containing coronavirus that has been selectedin vivo for extreme neurovirulence. This virus encodes spike (S)glycoproteins that are extraordinarily effective mediators ofintercellular membrane fusion, unique in their ability to initiatefusion even without prior interaction with the primary MHV receptor,a murine carcinoembryonic antigen-related cell adhesion molecule(CEACAM). In considering the possible role of this hyperactivemembrane fusion activity in neurovirulence, we discovered thatthe growth of JHM in tissue culture selected for variants thathad lost murine CEACAM-independent fusion activity. Among thecollection of variants, mutations were identified in regions encodingboth the receptor-binding (S1) and fusion-inducing (S2) subunitsof the spike protein. Each mutation was separately introducedinto cDNA encoding the prototype JHM spike, and the set of cDNAswas expressed using vaccinia virus vectors. The variant spikeswere similar to that of JHM in their assembly into oligomers,their proteolysis into S1 and S2 cleavage products, their transportto cell surfaces, and their affinity for a soluble form of murineCEACAM. However, these tissue culture-adapted spikes were significantlystabilized as S1-S2 heteromers, and their entirely CEACAM-dependentfusion activity was delayed or reduced relative to prototype JHMspikes. The mutations that we have identified therefore pointto regions of the S protein that specifically regulate the membranefusion reaction. We suggest that cultured cells, unlike certainin vivo environments, select for S proteins with delayed, CEACAM-dependentfusion activities that may increase the likelihood of virus internalizationprior to the irreversible uncoatingprocess.

^* Corresponding author. Mailing address: Department of Microbiology and Immunology, Loyola University Medical Center, 2160 SouthFirst Ave., Maywood, IL 60153. Phone: (708) 216-4850. Fax: (708)216-9574. E-mail: tgallag{at}luc.edu.

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