Pathogenicity of Different Rabies Virus Variants Inversely Correlates with Apoptosis and Rabies Virus Glycoprotein Expression in Infected Primary Neuron Cultures

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Journal of Virology, January 1999, p. 510-518, Vol. 73, No. 1
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.

Pathogenicity of Different Rabies Virus Variants Inversely Correlates with Apoptosis and Rabies Virus Glycoprotein Expression in Infected Primary Neuron Cultures

Kinjiro Morimoto,¹ D. Craig Hooper,¹ Sergei Spitsin,² Hilary Koprowski,¹ and Bernhard Dietzschold¹^,^*

Center for Neurovirology, Department of Microbiology and Immunology,¹ and Biotechnology Foundation Laboratories,² Thomas Jefferson University, Philadelphia, Pennsylvania 19107-6799

Received 30 July 1998/Accepted 23 September 1998

The mouse-adapted rabies virus strain CVS-24 has stable variants, CVS-B2c and CVS-N2c, which differ greatly in their pathogenicityfor normal adult mice and in their ability to infect nonneuronalcells. The glycoprotein (G protein), which has previously beenimplicated in rabies virus pathogenicity, shows substantial structuraldifferences between these variants. Although prior studies haveidentified antigenic site III of the G protein as the major pathogenicitydeterminant, CVS-B2c and CVS-N2c do not vary at this site. Thepossibility that pathogenicity is inversely related to G proteinexpression levels is suggested by the finding that CVS-B2c, theless pathogenic variant, expresses at least fourfold-higher levelsof G protein than CVS-N2c in infected neurons. Although thereis some difference between CVS-B2c- and CVS-N2c-infected neuronsin G protein mRNA expression levels, the differential expressionof G protein appears to be largely determined by posttranslationalmechanisms that affect G protein stability. Pulse-chase experimentsindicated that the G protein of CVS-B2c is degraded more slowlythan that of CVS-N2c. The accumulation of G protein correlatedwith the induction of programmed cell death in CVS-B2c-infectedneurons. The extent of apoptosis was considerably lower in CVS-N2c-infectedneurons, where G protein expression was minimal. While nucleoprotein(N protein) expression levels were similar in neurons infectedwith either variant, the transport of N protein into neuronalprocesses was strongly inhibited in CVS-B2c-infected cells. Thus,downregulation of G protein expression in neuronal cells evidentlycontributes to rabies virus pathogenesis by preventing apoptosisand the apparently associated failure of the axonal transportof Nprotein.

^* Corresponding author. Mailing address: Center for Neurovirology, Department of Microbiology and Immunology, Thomas JeffersonUniversity, 1020 Locust St., Philadelphia, PA 19107-6799. Phone:(215) 503-4692. Fax: (215) 923-7145. E-mail: bdietzschold{at}reddi1.uns.tju.edu.

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