Retargeting of coronavirus by substitution of the spike glycoprotein ectodomain: Crossing the host cell species barrier

被引:286
作者
Kuo, LL
Godeke, GJ
Raamsman, MJB
Masters, PS
Rottier, PJM
机构
[1] New York State Dept Hlth, Wadsworth Ctr Labs & Res, David Axelrod Inst, Albany, NY 12201 USA
[2] Univ Utrecht, Fac Vet Med, Dept Immunol & Infect Dis, Inst Virol, NL-3584 CL Utrecht, Netherlands
[3] Univ Utrecht, Inst Biomembranes, NL-3584 CL Utrecht, Netherlands
关键词
D O I
10.1128/JVI.74.3.1393-1406.2000
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
Coronaviruses generally have a narrow host range, infecting one or just a few species. Using targeted RNA recombination, we constructed a mutant of the coronavirus mouse hepatitis virus (MHV) in which the ectodomain of the spike glycoprotein (S) was replaced with the highly divergent ectodomain of the S protein of feline infectious peritonitis virus. The resulting chimeric virus, designated fMHV, acquired the ability to infect feline cells and simultaneously lost the ability to infect murine cells in tissue culture. This reciprocal switch of species specificity strongly supports the notion that coronavirus host cell range is determined primarily at the level of interactions between the S protein and the virus receptor. The isolation of fMHV allowed the localization of the region responsible for S protein incorporation into virions to the carboxy-terminal 64 of the 1,324 residues of this protein. This establishes a basis for further definition of elements involved in virion assembly. In addition, fMHV is potentially the ideal recipient virus for carrying out reverse genetics of MHV by targeted RNA recombination, since it presents the possibility of selecting recombinants, no matter how defective, that have regained the ability to replicate in murine cells.
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收藏
页码:1393 / 1406
页数:14
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