Neurodegenerative disease induced by the wild mouse ecotropic retrovirus is markedly accelerated by long terminal repeat and gag-pol sequences from nondefective Friend murine leukemia virus.

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J Virol. 1990 April; 64(4): 1648-1656

Neurodegenerative disease induced by the wild mouse ecotropic retrovirus is markedly accelerated by long terminal repeat and gag-pol sequences from nondefective Friend murine leukemia virus.

J L Portis, S Czub, C F Garon and F J McAtee

Laboratory of Persistent Viral Diseases, National Institute of Allergy and Infectious Diseases, Hamilton, Montana 59840.

ABSTRACT

The wild mouse ecotropic retrovirus (WM-E) induces a spongiformneurodegenerative disease in mice after a variable incubationperiod of 2 months to as long as 1 year. We isolated a molecularclone of WM-E (15-1) which was weakly neurovirulent (incidence,8%) but was highly leukemogenic (incidence, 45%). Both lymphoidand granulocytic leukemias were observed, and these leukemiaswere often neuroinvasive. A chimeric virus was constructed containingthe env and 3' pol sequences of 15-1 and long terminal repeat(LTR), gag, and 5' pol sequences from a clone of Friend murineleukemia virus (FB29). FB29 has been shown previously to replicateto high levels in the central nervous system (CNS) but is notitself neurovirulent. This finding was confirmed at the DNAlevel in the current study. Surprisingly, intraperitoneal inoculationof neonatal IRW mice with the chimeric virus (FrCasE) causedan accelerated neurodegenerative disease with an incubationperiod of only 16 days and was uniformly fatal by 23 days postinoculation.Introduction of the LTR of 15-1 into the FrCasE genome yieldeda virus (FrCasEL) with a degree of neurovirulence intermediatebetween those of 15-1 and FrCasE. No differences were foundin the levels of viremia or the relative levels of viral DNAin the spleens of mice inoculated with 15-1, FrCasE, or FrCasEL.However, the levels of viral DNA in the CNS correlated withthe relative degrees of neurovirulence of the respective viruses(FrCasE greater than FrCasEL greater than 15-1). Thus, the envand 3' pol sequences of WM-E (15-1) were required for neurovirulence,but elements within the LTR and gag-pol regions of FB29 hada profound influence on the level of CNS infection and the rateof development of neurodegeneration.

J Virol. 1990 April; 64(4): 1648-1656

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