Lymphatic Dissemination and Comparative Pathology of Recombinant Measles Viruses in Genetically Modified Mice

doi:10.1128/JVI.74.3.1364-1372.2000

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Journal of Virology, February 2000, p. 1364-1372, Vol. 74, No. 3
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Lymphatic Dissemination and Comparative Pathology of Recombinant Measles Viruses in Genetically Modified Mice

Branka Mrkic,¹ Bernhard Odermatt,² Michael A. Klein,³ Martin A. Billeter,¹ Jovan Pavlovic,⁴ and Roberto Cattaneo¹^,⁵^,^*

Molecular Biology Institute,¹ Pathology Institute,² Neuropathology Institute,³ and Medical Virology Institute,⁴ University of Zurich, Zurich, Switzerland, and Molecular Medicine Program, Mayo Clinic, Rochester, Minnesota⁵

Received 23 July 1999/Accepted 20 October 1999

The dissemination of the Edmonston measles virus (Ed-MV) vaccine strain was studied with genetically modified mice defectivefor the alpha/beta interferon receptor and expressing human CD46with human-like tissue specificity and efficiency. A few daysafter intranasal infection, macrophages expressing Ed-MV RNA weredetected in the lungs, in draining lymph nodes, and in the thymus.In lymph nodes, large syncytia which stained positive for viralRNA and for macrophage surface marker proteins were found andapoptotic cell death was monitored. In the thymus, smaller syncytiawhich stained positive for macrophage and dendritic cell markerswere detected. Thus, macrophages appear to be the main vectorsfor dissemination of MV infection in these mice; human macrophagesmay have a similar function in the natural host. We then comparedthe pathogenicities of two recombinant viruses lacking the C orV nonstructural proteins to that of the parental strain, Ed-MV.These viruses were less effective in spreading through the lymphaticsystem and, unlike Ed-MV, were not detected in the liver. Afterintracerebral inoculation the recombinant viruses caused lethaldisease less often than Ed-MV and induced distinctive patternsof gliosis and inflammation. Ed-MV was reisolated from brain tissue,but its derivatives were not. C- and V-defective viruses shouldbe considered as more-attenuated MV vaccinecandidates.

^* Corresponding author. Mailing address: Molecular Medicine Program, Mayo Clinic, Guggenheim 18, 200 First St. SW, Rochester,MN 55905. Phone: (507) 284-0171. Fax: (507) 266-4797. E-mail:cattaneo.roberto{at}mayo.edu.

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